Animal Models of DiseaseAnimal Welfare Information Center
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Compiled By:
Tim Allen
Animal Welfare Information Center, Information Centers Branch
National Agricultural Library, Agricultural Research Service, U. S. Department of Agriculture
10301 Baltimore Ave., Beltsville, Maryland 20705-2351
Allen, Tim Animal models of disease : January 1988-January 1995. (Quick bibliography series ; 95-14) 1. Diseases--Animal models--Bibliography. 2. Animal models in research--Bibliography. 3. Laboratory animals-- Bibliography. I. Title. aZ5071.N3 no.95-14
Line Description ---- ----------- 1. animal(W)model? 2. disease? or disorder? or syndrome? 3. S1 and S2 4. S3 and PY=1988:1995
1 NAL Call. No.: 381 J8282 Aberrant hypothalamic-pituitary-ovarian axis in the Watanabe heritable hyperlipidemic rabbit. Robins, E.D.; Nelson, L.M.; Hoeg, J.M. Bethesda, Md. : Lipid Research, inc., 1959-; 1994 Jan. Journal of lipid research v. 35 (1): p. 52-59; 1994 Jan. Includes references. Language: English Descriptors: Rabbits; Hyperlipemia; Animal models; Disease models; Hypercholesterolemia; Hypothalamus; Pituitary; Ovaries; Pituitary-gonadal axis; Low density lipoprotein; Receptors; Fsh; Lh; Progesterone; Estradiol; Gonadotropins; Cholesterol; Blood lipids Abstract: The WHHL rabbit has a defective low density lipoprotein receptor and is a model for familial hypercholesterolemia. WHHL rabbits are less fecund than NZW rabbits, the strain into which the defect has been inbred. This lower fecundity could be related to impaired ovarian steroidogenesis due to reduced intracellular availability of cholesterol. Here we compare the WHHL and NZW rabbits with regard to oocyte morphology and fertilization rates after stimulation with equine chorionic gonadotropin. We also compare hypothalamic-pituitary-ovarian axis function by measuring baseline and gonadotropin releasing hormone- stimulated plasma estradiol, progesterone, and gonadotropin levels, both before and after simvastatin inhibition of de novo cholesterol synthesis. WHHL rabbit oocytes remained encased in cumulus and had a lowered fertilization rate (9/50 vs. 83/87, P < 0.05). WHHL rabbits had lower baseline estradiol levels (7.1 +/- 0.72 vs. 10.2 +/- 0.94, P < 0.05) and had higher baseline follicle stimulating hormone (P < 0.05) and luteinizing hormone (P < 0.05) levels. Simvastatin lowered luteal progesterone concentrations only in WHHL rabbits (P < 0.05). We conclude that the hypothalamic- pituitary-ovarian axis in WHHL rabbits is abnormal. The reduced availability of intracellular cholesterol for progesterone synthesis by inhibition of de novo cholesterol biosynthesis leads to a significant reduction in plasma progesterone concentrations in the WHHL. These findings have implications for women with familial hypercholesterolemia, particularly regarding treatment with inhibitors of de novo cholesterol synthesis. 2 NAL Call. No.: 500 N21P Abnormal class I assembly and peptide presentation in the nonobese diabetic mouse. Li, F.; Guo, J.; Fu, Y.; Yan, G.; Faustman, D. Washington, D.C. : National Academy of Sciences,; 1994 Nov08. Proceedings of the National Academy of Sciences of the United States of America v. 91 (23): p. 11128-11132; 1994 Nov08. Includes references. Language: English Descriptors: Mice; Diabetes; T lymphocytes; Major histocompatibility complex; Histocompatibility antigens; Autoimmunity; Autoimmune diseases; Structural genes; Alleles; Gene expression; Animal models Abstract: Presentation of self-antigens by major histocompatibility compatibility complex (MHC) class I molecules requires the function MHC class II-linked genes Tap-1 and Tap-2. Evidence suggests that interruption of self- peptide presentation results in reduced cell surface expression of MHC class I molecules and the interruption correlates with progression to diabetic autoimmunity in nonobese diabetic (NOD) mice and humans. NOD mice possess a rare Tap-1 allele (Tap-1b); this is associated with reduced Tap-1 mRNA abundance in lymphocytes from diabetes-prone females and decreased conformationally correct class I molecules on the cell surface. In this study, we demonstrate that, similar to lymphoma cell lines with mutations in Tap-1 or Tap-2, the reduced expression of class I molecules on the surface of lymphocytes from diabetes-prone female NOD mice was normalized by incubation at low temperatures or by exposure to class I allele-specific peptides. As would be expected for cells that express surface class I molecules not associated with peptide, female NOD lymphocytes were resistant to lysis by class I-restricted, peptide-specific cytotoxic T lymphocytes. Furthermore, the rate of class I exit from the endoplasmic reticulum of lymphocytes from female NOD mice was delayed as demonstrated by delayed glycosylation. Male NOD mice, which are not prone to diabetes, lacked these functional defects in class I assembly and had near-normal levels of Tap-1 mRNA and exhibited normal density of class I epitopes that were peptide filled. These results are consistent with the possibility that the rare Tap-1b allele is associated with a quantitative defect in Tap-1 expression that influences disease course. 3 NAL Call. No.: RC628.A1O2 Abnormalities of plasma lipoproteins in a new genetically obese rat with non-insulin-dependent diabetes mellitus (Wistar fatty rat). Jiao, S.; Matsuzawa, Y.; Matsubara, K.; Kubo, M.; Tokunaga, K.; Odaka, H.; Ikeda, H.; Matsuo, T.; Tarui, S. Basingstoke, Hampshire : The Macmillan Press Ltd; 1991 Jul. International journal of obesity v. 15 (7): p. 487-495; 1991 Jul. Includes references. Language: English Descriptors: Obesity; Diabetes mellitus; Insulin; Cholesterol acyltransferase; Lipoproteins; Apolipoproteins; Blood plasma; Diet; Intestinal absorption; Rats Abstract: We investigated plasma lipoprotein profiles and the activities of tissue cholesterol regulating enzymes in Wistar fatty rats, an animal model for non-insulin-dependent diabetes mellitus (NIDDM). Wistar fatty rats were made by transfer of the fa gene to the Wistar Kyoto rats by backcross-breeding. Wistar fatty and control non-diabetic littermates were given a laboratory chow or an atherogenic diet containing 1 percent (weight percent) cholesterol, 0.5 percent cholic acid, and 5 percent lard. Under the chow diet, plasma fasting glucose and immunoreactive insulin concentrations in Wistar fatty rats were 1.5- and 6-fold higher than controls, respectively. Plasma cholesterol was significantly increased in Wistar fatty rats compared with controls. Elevated plasma cholesterol levels in Wistar fatties was accounted for by the increases of cholesterol content in the d < 1.006 g/ml lipoprotein and high-density lipoproteins. Under the atherogenic diet, plasma cholesterol levels in Wistar fatties were further increased by 129 percent compared with controls. The diet-induced increase of cholesterol contents was shown in all lipoprotein classes for Wistar fatty rats. The activities of regulatory enzymes for cholesterol biosynthesis or absorption were measured in Wistar fatty rats. Both hepatic and intestinal 3-hydroxy-3- methylglutaryl (HMG)-CoA reductase activities were significantly higher in Wistar fatty rats than those in controls (P < 0.05 and P < 0.01, respectively). ACAT activities in Wistar fatties were significantly increased in the intestine (P < 0.05) and decreased in the liver in comparison with controls (P < 0.01). Cholesterol loading caused suppression of HMG-CoA reductase activities and enhancement of ACAT activities of both tissues in Wistar fatty rats as much as in controls. These data suggest that hypercholesterolemia in the NIDDM rats might be attributed to the increases in both de novo synthesis and intestinal absorption of cholesterol. Magnified response of 4 NAL Call. No.: RA784.A1I5 Activity-induced anorexia in rats does not affect hypothalamic neuropeptide gene expression chronically. Wong, M.L.; Licinio, J.; Gold, P.W.; Glowa, J. New York, N.Y. : John Wiley & Sons; 1993 May. The International journal of eating disorders v. 13 (4): p. 399-405; 1993 May. Includes references. Language: English Descriptors: Physical activity; Anorexia; Hypothalamus; Neuropeptides; Gene expression; Rats Abstract: Hypothalamic neuropeptides are thought to contribute to the pathophysiology of eating disorders. In an animal model with chronic abnormalities of energy expenditure, appetitive behavior, and body weight, without acute food restriction, we found alterations in peripheral levels of adrenocorticotropic hormone and corticosterone, but no alterations in the expression of neuropeptides genes that are known to regulate ingestive behavior and food intake acutely. Our data suggest that activation of hypothalamic-pituitary- adrenal function in activity anorexia may not be due to increased transcription of corticotropin-releasing hormone gene, but might be related to posttranscriptional events or to other neuropeptides, such as arginine vasopressin. Furthermore, we suggest that abnormalities in neuropeptides observed in eating disorders may be caused by acute food restriction, rather than by chronic hyperactivity, anorexia, and low weight. 5 NAL Call. No.: 381 J824 Adipose cell hyperplasia and enhanced glucose disposal in transgenic mice overexpressing GLUT4 selectively in adipose tissue. Shepherd, P.R.; Gnudi, L.; Tozzo, E.; Yang, H.; Leach, F.; Kahn, B.B. Baltimore, Md. : American Society for Biochemistry and Molecular Biology; 1993 Oct25. The Journal of biological chemistry v. 268 (30): p. 22243-22246; 1993 Oct25. Includes references. Language: English Descriptors: Mice; Transgenic animals; Animal proteins; Glucose; Active transport; Plasma membranes; Adipocytes; Hyperplasia; Adipose tissue; Carbohydrate metabolism; Brown fat; Body fat; Glucose tolerance Abstract: To gain insight into the molecular pathogenesis of obesity and specifically the role of nutrient partitioning in the development of obesity, we overexpressed the insulin- responsive glucose transporter (GLUT4) in transgenic mice under the control of the fat-specific aP2 fatty acid-binding protein promoter/enhancer. Two lines of transgenic mice were generated, which overexpressed GLUT4 6-9-fold in white fat and 3-5-fold in brown fat with no overexpression in other tissues. In vivo glucose tolerance was enhanced in transgenic mice. In isolated epididymal, parametrial, and subcutaneous adipose cells from transgenic mice, basal glucose transport was 20-34- fold greater than in nontransgenic littermates. Insulin- stimulated glucose transport was 2-4-fold greater in cells from transgenic mice. Total body lipid was increased 2-3-fold in transgenic mice overexpressing GLUT4 in fat. Surprisingly, fat cell size was unaltered and fatcell number was increased >2-fold. This is the first animal model in which increased fat mass results solely from adipocyte hyperplasia and it will be a valuable model for understanding the mechanisms responsible for fat cell replication and/or differentiation in vivo. 6 NAL Call. No.: 421 J828 Aedes (Gymnometopa) mediovittatus (Diptera: Culicidae) as an experimental vector of Brugia pahangi and B. malayi (Spirurida: Filariidae). Trpis, M. Lanham, Md. : The Entomological Society of America; 1994 May. Journal of medical entomology v. 31 (3): p. 442-444; 1994 May. Includes references. Language: English Descriptors: Aedes mediovittatus; Brugia malayi; Brugia pahangi; Disease vectors; Experimental infection; Susceptibility; Animal models; Filariasis Abstract: To test the susceptibility of Aedes (Gymnometopa) mediovittatus to infection with Brugia pahangi and Brugia malayi, females originating from the suburbs of San Juan, Puerto Rico, were fed on infected gerbils (Meriones unguiculatus). On average, 39.2% of the Ae. mediovittatus females became infected with L3 larvae of B. pahangi and 47.4% with B. malayi. The average number of infective L3 larvae of B. pahangi and B. malayi dissected from mosquitoes was 2.6 +/- 1.2 and 2.9 +/- 1.0, respectively. The largest number of in a single mosquito was 16. After 10 d of development in the mosquitoes, L3 larvae of both Brugian species were found in greatest number in the thorax, in lesser number in the head/proboscis, and in least number in the abdomen. Ae. mediovittatus may, serve as a useful laboratory model for the study of genetic susceptibility and refractoriness of mosquito vectors to filarial parasites. 7 NAL Call. No.: 41.8 P27 Age-related changes in the prostate and testes of the beagle dog. Lowseth, L.A.; Gerlach, R.F.; Gillett, N.A.; Muggenburg, B.A. Lawrence, Kan. : American College of Veterinary Pathologists; 1990 Sep. Veterinary pathology v. 27 (5): p. 347-353; 1990 Sep. Includes references. Language: English Descriptors: Dogs; Prostate; Weight; Testes; Histology; Blood serum; Testosterone; Aging; Age differences; Animal models 8 NAL Call. No.: TX345.B74 Alcoholism and folate homeostasis. Halsted, C.H. San Diego, Calif. : Academic Press; 1989. Bristol-Myers Squibb/Mead Johnson nutrition symposia v. 7: p. 249-266. charts; 1989. In the series analytic: Nutrition and the Origins of Disease / edited by G.H. Halsted and R.B. Rucker. Literature review. Includes references. Language: English Descriptors: Folic acid; Alcoholism; Vitamin deficiencies; Nutrition physiology; Liver; Nutrient balance; Literature reviews Abstract: This chapter examines a variety of issues relating to folate deficiency and alcoholism: 1) incidence; 2) clinical significance (anemia, intestinal mucosa, hepatic injury and regeneration); 3) pathogenesis (dietary inadequacy, intestinal malabsorption; hepatobiliary metabolism, urinary excretion); and 4) animal models. 9 NAL Call. No.: SF601.J65 Alterations in carbohydrate metabolism in canine lymphoma. Vail, D.M.; Ogilvie, G.K.; Wheeler, S.L.; Fettman, M.J.; Johnston, S.D.; Hegstad, R.L. Hagerstown, Md. : American College of Veterinary Medicine; 1990 Jan. Journal of veterinary internal medicine v. 4 (1): p. 8-11; 1990 Jan. Includes references. Language: English Descriptors: Dogs; Lymphoma; Carbohydrate metabolism disorders; Blood sugar; Glucose tolerance; Blood serum; Lactic acid; Insulin; Cachexia; Disease models; Animal models 10 NAL Call. No.: 41.8 AM3 Alternatives to the use of conventional research animals in neoplasia research. Ladiges, W.C. Schaumburg, Ill. : The Association; 1992 Mar01. Journal of the American Veterinary Medical Association v. 200 (5): p. 674-676; 1992 Mar01. Paper presented at the symposium "Animal welfare and alternatives to animals--current knowledge and research needs", July 31, 1991, Seattle, Washington. Includes references. Language: English Descriptors: Animal testing alternatives; Medical research; Neoplasms; Animal models; Disease models 11 NAL Call. No.: 41.8 Am3 Alternatives to the use of conventional research animals in neoplasia research. Ladiges, W.C. \u University of Washington, Seattle, WA Schaumburg, Ill. : The Association; 1992 Mar01. Journal of the American Veterinary Medical Association v. 200 (5): p. 674-676; 1992 Mar01. Corrects AGRICOLA accession number IND92017402 in which the publication year was incorrectly entered as 1991. Paper presented at the symposium "Animal welfare and alternatives to animals--current knowledge and research needs", July 31, 1991, Seattle, Washington. Includes references. Language: English Descriptors: Animal testing alternatives; Medical research; Neoplasms; Animal models; Disease models 12 NAL Call. No.: QP141.A1J68 Amino acid availability and brain development: effects of nutritional and metabolic inadequacies. Huether, G. Basingstoke : The Macmillan Press Ltd; 1989. European journal of clinical nutrition v. 43 (suppl.1): p. 19-25; 1989. Includes 25 references. Language: English Descriptors: Amino acids; Bioavailability; Brain disorders; Hyperphenylalaninemia; Child development; Protein metabolism; Protein synthesis; Malnutrition; Neurotransmitters; Serotonin; Animal models; Man Abstract: Inadequacies of the brain's amino acid supply are relevant to the processes of protein accretion and transmitter synthesis during brain development. Experimental hyperphenylalaninaemia has demonstrated the consequences of rather severe imbalances of the brain's amino acid supply. An inadequate supply of essential amino acids has been shown to influence a variety of developmental processes. 13 NAL Call. No.: QP141.A1A63 Amino acid metabolism in human cancer cachexia. Pisters, P.W.T.; Brennan, M.F. Palo Alto, Calif. : Annual Reviews, Inc; 1990. Annual review of nutrition v. 10: p. 107-132. charts; 1990. Includes 138 references. Language: English Descriptors: Amino acid metabolism; Carcinoma; Cachexia; Nitrogen balance; Kinetics; Men; Women Abstract: Cancer cachexia is a complex syndrome that occurs with variable incidence in patients with solid tumors and those with hematologic malignancies. It is associated with characteristic physical and laboratory findings, and at a more fundamental level, with significant abnormalities in carbohydrate, lipid, and protein metabolism. These alterations in intermediary metabolism are demonstrable early in the syndrome, even before the onset of weight loss, when the more characteristic features of cancer cachexia are evident. Progressive wasting of peripheral protein stores is a major feature of cancer cachexia and often one of the most graphic realities of malignancy for patients and their families. Unfortunately, significant problems with the animal models of cancer cachexia make conclusions derived from animal studies difficult to extrapolate to humans. Data from human studies indicate that human cancer cachexia is associated with minimal aberrations in circulating free amino acid concentrations; increased whole-body protein turnover, synthesis, and catabolism; reduced rates of skeletal muscle protein synthesis; and increased rates of hepatic protein synthesis. Whether or not these alterations represent pathologic responses or physiologic adaptation by the host to the presence of malignancy remains to be seen. Future investigations must focus on more careful evaluation of interorgan amino acid metabolism, investigation of skeletal muscle protein catabolic rates in cancer cachexia, and definition of the roles of altered hormonal and cytokine regulation of these processes. Such studies will more precisely define the level at which amino acid metabolism is altered significantly and, we hope, permit more specific therapeutic intervention designed to reverse the debilitating effects of cancer cachexia. 14 NAL Call. No.: QP501.C6 An animal model of systemic carnitine deficiency produced by haemodialysis of sheep. Snoswell, A.M.; Fishlock, R.C.; Runciman, W.B.; Carapetis, R. Oxford : Pergamon Press; 1989. Comparative biochemistry and physiology : B : Comparative biochemistry v. 93 (4): p. 741-745; 1989. Includes references. Language: English Descriptors: Sheep; Models; Deficiency diseases; Carnitine; Hemodialysis 15 NAL Call. No.: TD172.J6 An animal model to assess the potential for viral disease transmission from lawns irrigated with wastewater. Deming, E.J.; Mote, C.R.; Von Bernuth, R.D.; Potgieter, L.N.D. New York, N.Y. : Marcel Dekker; 1992 Dec. Journal of environmental science and health : Part A : Environmental science and engineering v. 27 (8): p. 2199-2211; 1992 Dec. Includes references. Language: English Descriptors: Lawns and turf; Irrigation; Waste water; Contamination; Porcine enterovirus; Pigs; Disease transmission; Animal models; Disease models; Human diseases; Infection; Risk 16 NAL Call. No.: SF95.A1C6 Animal models for studies of relationships between diet and diabetes. Herberg, L. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 111-148; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Literature review. Includes references. Language: English Descriptors: Diabetes mellitus; Pancreas; Insulin; Pituitary hormones; Rats; Blood sugar; Dietary carbohydrate; Dietary fat; Animal models; Feed intake; Cricetulus barabensis; Hyperinsulinemia; Insulin secretion; Literature reviews 17 NAL Call. No.: QR180.3.D4 Animal models for the evaluation of drugs and vaccines for HIV infection and AIDS: report of a WHO working group. Esparza, J. Basel : S. Karger; 1990. Developments in biological standardization v. 72: p. 367-372; 1990. In the series analytic: Progress in animal retroviruses / edited by D. Gaudry and W. Hennessen. Meeting held on Oct 4-6, 1989, Annecy, France. Language: English Descriptors: Disease models; Human immunodeficiency virus; Acquired immune deficiency syndrome 18 NAL Call. No.: RC607.A26I63 1989 Animal models in AIDS. Schellekens, Huub; Horzinek, Marian C. Nederlandse Centrale Organisatie voor Toegepast- Natuurwetenschappelijk Onderzoek International TNO Meeting 1989 : Maastricht, Netherlands. Amsterdam ; New York : Elsevier ; New York, NY, USA : Sole distributors for the USA and Canada, Elsevier Science Pub. Co.,; 1990. xxii, 380 p. : ill. ; 25 cm. Includes index. Includes bibliographical references. Language: English Descriptors: AIDS (Disease) 19 NAL Call. No.: QL55.A53 1988 Animal models in biomedical research proceedings of symposium, 20-21 January 1988. Laboratory Animals Information Service Centre (India) Hyderabad, India : Laboratory Animals Information Service Centre, National Institute of Nutrition, Indian Council of Medical Research, [1988?]; 1988. 79 p., [7] p. of plates : ill. ; 25 cm. Symposium held in New Delhi, India. Includes bibliographical references. Language: English Descriptors: Animal models in research; Diseases 20 NAL Call. No.: QL55.F43 1987 Animal models in hemostasis and thrombosis. Rowsell, H.C. Dordrecht : M. Nijhoff; 1988. New developments in biosciences : their implications for laboratory animal science : proceedings of the Third Symposium, Amsterdam, The Nethrlands, 1-5 June 1987 / edited by Anton C. Beyneen and Henk A. Solleveld. p. 289-294; 1988. Includes references. Language: English Descriptors: Laboratory animals; Disease models; Thrombosis; Blood flow; Hemorrhage; Blood coagulation 21 NAL Call. No.: 475 EX7 Animal models in interferon research: some current trends. Schellekens, H. Basel : Birkhauser; 1989 Jun15. Experientia v. 45 (6): p. 558-562; 1989 Jun15. Literature review. Includes references. Language: English Descriptors: Animal experiments; Animal research; Interferon; In vivo; Disease models; Bacterial diseases; Protozoal infections; Parasites 22 NAL Call. No.: 41.8 Ad9 v.37 Animal models in liver research. Cornelius, Charles E. San Diego : Academic Press,; 1993. xx, 479 p. : ill. ; 24 cm. (Advances in veterinary science and comparative medicine ; v.37). Includes bibliographical references and index. Language: English Descriptors: Diseases 23 NAL Call. No.: QR1.F4 Animal models in the study of pathogenesis. Adlam, C. Amsterdam : Elsevier Science Publishers; 1988. FEMS symposium - Federation of European Microbiological Societies v. 40: p. 159-167; 1988. Includes references. Language: English Descriptors: Animals; Models; Pathogenesis; Bovine mastitis; Rhinitis; Lymphadenitis; Sheep; Respiratory diseases 24 NAL Call. No.: QP141.A1C8 Animal models of appetitive behavior: interaction of nutritional factors and drug seeking behavior. Kanarek, R.B.; Marks-Kaufman, R. New York, N.Y. : Wiley; 1988. Current concepts in nutrition v. 16: p. 1-5; 1988. Includes references. Language: English Descriptors: Feeding behavior; Appetite; Models; Nutrition; Drug effects; Interactions 25 NAL Call. No.: QP601.M49 Animal models of chronic ethanol toxicity. Lieber, C.S.; DeCarli, L.M. New York : Academic Press, 1955-; 1994. Methods in enzymology. p. 585-594; 1994. In the series analytic: Oxygen radicals in biological systems (Part C) / edited by L. Packer. Includes references. Language: English Descriptors: Ethanol; Toxicity; Chronic course; Diet; Liquid diets; Liver; Animal models; Papio; Rats 26 NAL Call. No.: SF95.A1C6 Animal models of diet-induced atherosclerosis. Clarkson, T.B.; Shively, C.A.; Weingand, K.W. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 56-82; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Includes references. Language: English Descriptors: Animal models; Experimental atherosclerosis; Atherogenic diet; Rabbits; Pigeons; Pigs; Primates; Pathogenesis 27 NAL Call. No.: aZ5071.N3 Animal models of disease 1979-August 1988. Swanson, J.C. Beltsville, Md. : The Library; 1988 Nov. Quick bibliography series - U.S. Department of Agriculure, National Agricultural Library (U.S.). (89-07): 25 p.; 1988 Nov. Bibliography. Language: English Descriptors: Animals; Disease models; Animal welfare; Bibliographies 28 NAL Call. No.: aZ5071.N3 Animal models of disease, January 1979-August 1989. Swanson, J.; Clingerman, K. Beltsville, Md. : The Library; 1989 Dec. Quick bibliography series - U.S. Department of Agriculure, National Agricultural Library (U.S.). (90-09): 27 p.; 1989 Dec. Updates QB 89-07. Bibliography. Language: English Descriptors: Animals; Laboratory animals; Animal diseases; Disease models; Bibliographies 29 NAL Call. No.: aZ5071.N3 Animal models of disease, January 1988-January 1994. Smith, C.P.; Larson, J.A. Beltsville, Md., National Agricultural Library; 1994 Mar. Quick bibliography series - National Agricultural Library (94-19): 83 p.; 1994 Mar. Updates QB 92-61. Language: English Descriptors: Animal models; Disease models; Bibliographies 30 NAL Call. No.: aZ5071.N3 Animal models of disease--January 1979-December 1990. Smith, C.P. Beltsville, Md. : The Library; 1991 Feb. Quick bibliography series - U.S. Department of Agriculture, National Agricultural Library (U.S.). (91-42): 38 p.; 1991 Feb. Updates QB 90-09. Bibliography. Language: English Descriptors: Animal models; Diseases; Bibliographies 31 NAL Call. No.: aZ5071.N3 Animal models of disease--January 1981-July 1992. Smith, C.P. Beltsville, Md. : The Library; 1992 Aug. Quick bibliography series - U.S. Department of Agriculture, National Agricultural Library (U.S.). (92-61): 59 p.; 1992 Aug. Updates QB 91-42. Language: English Descriptors: Animal diseases; Disease models; Bibliographies 32 NAL Call. No.: QR201.A37A55 1993 Animal models of HIV and other retroviral infections. Racz, Paul; Letvin, Norman L.; Gluckman, J. C. Basel ; New York : Karger,; 1993. viii, 200 p. : ill. (some col.) ; 25 cm. Includes bibliographical references and index. Language: English Descriptors: HIV infections; Retrovirus infections 33 NAL Call. No.: 500 N484 Animal models of human eating disorders. Smith, G.P. New York, N.Y. : The Academy; 1989. Annals of the New York Academy of Sciences v. 575: p. 63-74; 1989. In the series analytic: The psychology of human eating disorders: preclinical and clinical perspectives / edited by L.H. Schneider, S.J. Cooper, and K.A. Halmi. Literature review. Includes references. Language: English Descriptors: Nutritional disorders; Human nutrition research; Animal experiments; Anorexia nervosa; Bulimia nervosa; Models 34 NAL Call. No.: 41.8 Ad9 Animal models of liver fibrosis. Rojkind, M. \u Albert Einstein College of Medicine, Bronx, NY; Greenwel, P. San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 333-355; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Liver diseases; Animal models; Alcoholism; Schistosomiasis; Carbon tetrachloride 35 NAL Call. No.: 41.8 P27 Animal models of retrovirus-associated malignancies. Cremer, K.J.; Gruber, J. Lawrence, Kan. : American College of Veterinary Pathologists; 1992 Nov. Veterinary pathology v. 29 (6): p. 572-578; 1992 Nov. Includes references. Language: English Descriptors: Animal models; Retroviridae 36 NAL Call. No.: QH301.N32 Animal studies of iodized oils: iodine disposition and physiological effects. Chambon, C.; Chastin, I. New York, N.Y. : Plenum Press; 1993. NATO ASI series : Series A : Life sciences v. 241: p. 159-167; 1993. In the series analytic: Iodine deficiency in Europe: a continuing concern / edited by F. Delange, J.T. Dunn, and D. Glioner. Proceedings of an International Workshop, April 24-28, 1992, Brussels, Belgium. Includes a discussion, p. 166-167. Includes references. Language: English Descriptors: Cooking oils; Deficiency diseases; Goiter; Human diseases; Iodine; Physiopathology; Rats; Animal models; Livestock 37 NAL Call. No.: 41.8 Am3 Animals as a source of Escherichia coli pathogenic for human beings. Whipp, S.C.; Rasmussen, M.A.; Cray, W.C. Jr Schaumburg, Ill. : The Association; 1994 Apr15. Journal of the American Veterinary Medical Association v. 204 (8): p. 1168-1175; 1994 Apr15. Includes references. Language: English Descriptors: Cattle; Escherichia; Escherichia coli; Pathogenicity; Man; Disease prevalence; Animal models; Human diseases; Gastrointestinal diseases 38 NAL Call. No.: 389.1 W892 Antiarrhythmic effects of fish oils. Charnock, J.S. Basel : S. Karger; 1991. World review of nutrition and dietetics v. 66: p. 278-291; 1991. In the series analytic: Health effects of omega 3 polyunsaturated fatty acids in seafoods / edited by A.P. Simopoulos, R.R. Kifer, Martin, R.E. and S.M. Barlow. Includes references. Language: English Descriptors: Fish oils; Heart rate; Supplements; Animal models; Polyenoic fatty acids; Dietary fat; Muscle contraction; Animal experiments; Literature reviews 39 NAL Call. No.: QH426.T74 Atherosclerosis in mice: getting to the heart of a polygenic disorder. Rubin, E.M.; Smith, D.J. Cambridge, U.K. : Elsevier Trends Journals; 1994 Jun. Trends in genetics v. 10 (6): p. 199-203; 1994 Jun. Includes references. Language: English Descriptors: Mice; Atherosclerosis; Animal models; Transgenic animals; Genetic engineering; Apolipoproteins; High density lipoprotein; Literature reviews; Low density lipoprotein; Induced mutations Abstract: The mouse is being increasingly used as a model system for understanding the common and complex polygenic condition of atherosclerosis. Mice have been created in which genes involved in this condition have been overexpressed or have been altered by gene targeting. Here, we concentrate on recent experiments that use transgenic and gene knockout mice as an in vivo assay system to unravel the interactions between various genes involved in atherogenesis. We focus in particular on examples in which unique insights into the human condition have been derived from studies in mice. 40 NAL Call. No.: SF910.T8A86 Atlas of tumor pathology of the Fischer rat.. Fischer rat Stinson, Sherman F.,_1946-; Schuller, Hildegard M.; Reznik, Gerd Boca Raton, Fla : CRC Press,; 1990. 546 p. : ill. ; 27 cm. Includes bibliographical references and index. Language: English Descriptors: Tumors in animals; Atlases; Rats as laboratory animals; Atlases; Rats; Diseases; Atlases; Tumors; Animal models; Atlases 41 NAL Call. No.: 447.8 Am3 Atrial natriuretic peptide and glomerular hyperfiltration during onset of spontaneous diabetes mellitus. Okwueze, M.I.; Opgenorth, T.J.; Von Geldern, T.W.; Vari, R.C. Bethesda, Md. : American Physiological Society, 1898-; 1994 Feb. American journal of physiology v. 266 (2,pt.2): p. R572- R577; 1994 Feb. Includes references. Language: English Descriptors: Diabetes mellitus; Glomerular filtration rate; Peptides; Receptors; Antagonists; Hemodynamics; Kidneys; Rats Abstract: The mechanisms responsible for the elevation of glomerular filtration rate (GFR) in early stages of insulin- dependent diabetes mellitus (IDDM) are undefined. The objectives of this study were to define the temporal pattern of onset of glomerular hyperfiltration in the spontaneously diabetes-prone (BB/DP) rat and to evaluate the possible role of atrial natriuretic peptide (ANP) as the primary mediator of the observed alterations in renal hemodynamics. GFR was significantly higher (1.38 +/- 0.07 ml.min-1.g-1; n = 5) in moderately hyperglycemic BB/DP rats (blood glucose > 270 mg/dl) 14 days after the onset of IDDM compared with age- matched diabetes-resistant rats (BB/DR), which averaged 1.03 +/- 0.07 ml.min-1.g-1 (n = 7). Circulating ANP levels in moderately hyperglycemic BB/DP rats 1, 7, and 14 days after onset of IDDM were within the normal range, averaging 100 +/- 21, 57 +/- 12, and 65 +/- 6 pg/ml, respectively, and were not significantly different (P > 0.05) from ANP levels in age- matched normoglycemic BB/DR rats. To further test the role of ANP in glomerular hyperfiltration, an ANP receptor antagonist was infused into anesthetized BB/DP rats (n = 10) 14 days after onset of IDDM, after baseline measurements of mean arterial pressure, renal hemodynamics, and renal fluid and electrolyte excretions. ANP receptor antagonism caused a significant reduction in mean arterial pressure from 120 +/- 3 to 103 +/- 2 mmHg; however, there were no significant effects of ANP receptor blockade on GFR. These results indicate that 1) glomerular hyperfiltration occurs within the first 2 wk after onset of IDDM in the moderately hyperglycemic BB/DP rat and 2) ANP is not the primary mediator of glomerular hyperfiltration during the onset of diabetes in this animal model of spontaneous IDDM. 42 NAL Call. No.: 448.8 V81 Attenuating mutations in the E2 glycoprotein gene of Venezuelan equine encephalitis virus: construction of single and multiple mutants in a full-length cDNA clone. Davis, N.L.; Powell, N.; Greenwald, G.F.; Willis, L.V.; Johnson, B.J.B.; Smith, J.F.; Johnston, R.E. Duluth, Minn. : Academic Press; 1991 Jul. Virology v. 183 (1): p. 20-31; 1991 Jul. Includes references. Language: English Descriptors: Venezuelan equine encephalitis virus; Mutants; Mutations; Clones; Phenotypes; Live vaccines; Attenuation; Glycoproteins; Genes; Virulence; Immune response; Pathogenesis Abstract: Attenuated mutants of Venezuelan equine encephalitis virus (VEE) were isolated by selection for rapid penetration of cultured cells (R.E.Johnston and J.F. Smith, 1988, Virology 162, 437-443). Sequence analysis of these mutants identified candidate attenuating mutations at four loci in the VEE E2 glycoprotein gene: a double mutation at E2 codons 3 and 4, and single substitutions at E2 76, 120, and 209. Each candidate mutation was reproduced in an isogenic recombinant VEE strain using site-directed mutagenesis of a full-length cDNA clone of VEE. Characterization of these molecularly cloned mutant viruses showed that mutation at each of the four loci in the E2 gene was sufficient to confer both the accelerated penetration and attenuation phenotypes. Inoculation of the molecularly cloned viruses into rodent models that differ in their response to VEE suggested that individual mutations affected different aspects of VEE pathogenesis. Full-length clones containing multiple mutations were produced by combining independently attenuating mutations. Molecularly cloned viruses carrying two or three mutations were more attenuated in sensitive animal models than viruses which contained any single mutation alone. However, these highly attenuated strains still retained the ability to induce an immune response sufficient to protect against a high dose challenge with virulent VEE. These results indicate that production of a molecularly cloned live virus vaccine for VEE is feasible. 43 NAL Call. No.: 41.8 Ad9 Avian fatty liver hemorrhagic syndrome: a comparative review. Hansen, R.J. \u University of California, Davis, CA; Walzem, R.L. San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 451-468; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Hens; Fatty liver; Fatty liver hemorrhagic syndrome; Animal models; Lipid metabolism; Transport; Pathogenesis; Man; Cows; Cats; Literature reviews 44 NAL Call. No.: HV5285.A43 Behavioral animal models in alcohol abuse research. Grant, K.A. Washington, D.C. : U.S. Department of Health and Human Services; 1990. Alcohol health and research world - National Institute on Alcohol Abuse and Alcoholism v. 14 (3): p. 187-192; 1990. Includes references. Language: English Descriptors: Alcoholism; Drinking behavior; Animal experiments; Laboratory animals; Animal models 45 NAL Call. No.: 500 N21P beta-Cell lipotoxicity in the pathogenesis of non-insulin- dependent diabetes mellitus of obese rates: Impairment in adipocyte-beta-cell relationships. Lee, Y.; Hirose, H.; Ohneda, M.; Johnson, J.H.; McGarry, J.D.; Unger, R.H. Washington, D.C. : National Academy of Sciences,; 1994 Nov08. Proceedings of the National Academy of Sciences of the United States of America v. 91 (23): p. 10878-10882; 1994 Nov08. Includes references. Language: English Descriptors: Rats; Diabetes mellitus; Pancreas islets; Pathogenesis; Blood lipids; Fatty acids; Hyperglycemia; Insulin secretion; Lipid metabolism disorders; Animal models; Obesity; Experimental diabetes Abstract: Hyperinsulinemia, Ioss of glucose-stimulated insulin secretion (GSIS), and peripheral insulin resistance coexist in non-insulin-dependent diabetes mellitus (NIDDM). Because free fatty acids (FFA) can induce these same abnormalities, we studied their role in the pathogenesis NIDDM of obese Zucker diabetic fatty (ZDF-drt) rats from 5 weeks of age (before the onset of hyperglycemia) until 14 weeks. Two weeks prior to hyperglycemia, plasma FFA began to rise progressively, averaging 1.9 + 0.06 mM at the onset of hyperglycemia (P < 0.001 vs. controls). At this time GSIS was absent and beta-cell GLUT-2 glucose transporter was decreased. The triacylglycerol content of prediabetic islets rose to 10 times that of controls and was correlated with plasma FFA (r = 0.825; P < 0.001), which, in turn. was correlated with the plasma glucose concentration (r = 0.873; P < 0.001). Reduction of hyperlipacidemia to 1.3 +/- 0.07 mM by pair feeding with lean littermates reduced all beta-cell abnormalities and prevented hyperglycemia. Normal rat islets that had been cultured for 7 days in medium containing 2 mM FFA exhibited increased basal insulin secretion at 3 mM glucose, and first- phase GSIS was reduced by 68%; in prediabetic islets, first- phase GSIS was reduced by 69% by FFA. The results suggest a role for hyperlipacidemia in the pathogenesis of NIDDM: resistance to insulin-mediated antilipolysis is invoked to explain the high FFA despite hyperinsulinemia, and sensitivity of beta cells to hyperlipacidemia is invoked to explain the FFA-induced loss of GSIS. 46 NAL Call. No.: 41.8 Ad9 Biliary atresia in lampreys. Youson, J.H. \u University of Toronto, Ontario, Canada San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 197-255; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Liver diseases; Atresia; Liver; Lampreys; Bile ducts; Life cycle; Animal models; Literature reviews 47 NAL Call. No.: TP248.2.B55126 1993 Biotechnology and safety assessment. Thomas, J. A._1933-; Myers, Laurie A. New York : Raven Press,; 1993. ix, 270 p. : ill. ; 25 cm. Includes bibliographical references and index. Language: English Descriptors: Biotechnology; Health risk assessment 48 NAL Call. No.: QL55.F43 1987 Blastomere karyotyping: a direct method for producing mouse trisomy 16 less than leads to diploid aggregation chimeras as an animal model of human down's syndrome. Bacchus, C.; Buselmaier, W. Dordrecht : M. Nijhoff; 1988. New developments in biosciences : their implications for laboratory animal science : proceedings of the Third Symposium, Amsterdam, The Nethrlands, 1-5 June 1987 / edited by Anton C. Beyneen and Henk A. Solleveld. p. 405-408. ill; 1988. Includes references. Language: English Descriptors: Mice; Blastomere; Karyotypes; Trisomy; Diploidy; Chimeras; Disease models; Down's syndrome 49 NAL Call. No.: QR360.J6 Borna disease virus in mice: host-specific differences in disease expression. Rubin, S.A.; Waltrip, R.W. II; Bautista, J.R.; Carbone, K.M. Washington, D.C. : American Society for Microbiology; 1993 Jan. Journal of virology v. 67 (1): p. 548-552; 1993 Jan. Includes references. Language: English Descriptors: Mice; Bo RNAdisease virus; Animal models; Experimental infections; Immunopathology; Antibody formation; Inflammation; Strain differences; Encephalitis; Abnormal behavior Abstract: We developed a mouse model of Borna disease to facilitate immunopathogenesis research by adaptation of Borna disease virus to mice through serial passage in mouse brain tissue. Borna disease virus replication, antibody production, inflammation, and Borna disease expression in several different strains of mice were examined. 50 NAL Call. No.: QR360.J6 Bovine leukemia virus, an animal model for the study of intrastrain variability. Willems, L.; Thienpont, E.; Kerkhofs, P.; Burny, A.; Mammerickx, M.; Kettmann, R. Washington, D.C. : American Society for Microbiology; 1993 Feb. Journal of virology v. 67 (2): p. 1086-1089; 1993 Feb. Includes references. Language: English Descriptors: Sheep; Bovine oncovirus; Genetic variation; Structural genes; Viral proteins; Repetitive DNA; Nucleotide sequences; Strain differences; Mutations Abstract: Intradermal injection of a cloned bovine leukemia virus (BLV) provirus (pV344) into sheep allowed direct evaluation of intrastrain variability. A sheep was injected with pV344 DNA mixed with DEAE-dextran and became persistently infected with BLV strain 344. After 18 months, DNA was extracted from peripheral blood leukocytes from a single 0.5- ml blood sample. The long terminal repeat (LTR) and the env gene were amplified by using the polymerase chain reaction, cloned, and sequenced. Nineteen independent LTR clones (0.6-kb inserts) and 16 env clones (1-kb inserts) were analyzed. The in vivo rate of nucleotide change was 0.009%/year (two mutations out of 14,464 bp in 1.5 years), corresponding to only one amino acid change in the env gene. Five point mutations (all transitions), corresponding to a modification rate of 0.034%/year (five mutations out of 9,709 bp in 1.5 years), were identified in the LTR. As a control for Taq DNA polymerase errors, the same procedure using pV344 plasmid DNA was carried out. Out of 9,944 bp sequenced, three point mutations were found (i.e., one misincorporation in 3,315 nucleotides). These data demonstrate the extremely low level (or absence) of intrastrain variability of BLV in vivo. Consequently, BLV persistence in the infected host does not seem to result from an escape mutant strategy, in sharp contrast with the high mutation rates observed in the lentivirus family. The lack of genetic variation supports the possibility of successful vaccine against BLV and probably against the related human T-cell leukemia viruses. 51 NAL Call. No.: SF601.C66 Bovine leukemia virus. III. Zoonotic potential, molecular epidemiology, and an animal model. Johnson, R. Trenton, N.J. : Veterinary Learning Systems Company, Inc; 1991 Oct. The Compendium on continuing education for the practicing veterinarian v. 13 (10): p. 1631-1640; 1991 Oct. Literature review. Includes references. Language: English Descriptors: Dairy cattle; Bovine oncovirus; Zoonoses; Risk; Molecular biology; Epidemiology; Disease models; Animal models; Human diseases; Leukemia; Literature reviews 52 NAL Call. No.: QP141.A1P72 Brain iron: location and function. Beard, J.L.; Connor, J.D.; Jones, B.C. Tarrytown, N.Y. : Pergamon Press; 1993 Jul. Progress in food & nutrition science v. 17 (3): p. 183-221; 1993 Jul. Includes references. Language: English Descriptors: Iron; Brain; Nutrition physiology; Mental ability; Mineral deficiencies; Tissues; Mineral content; Blood picture; Central nervous system; Animal models; Ferritin; Transferrin; Multiple sclerosis; Alzheimer's disease; Parkinson's disease; Neurotransmitters; Human behavior; Neuroleptics; Literature reviews Abstract: This review has a focus on the distribution and function of iron in human brain and appropriate animal models. Data are presented on the consequences of abnormalities of iron status with regard to neural development, neurotransmitter metabolism, and cognition. 53 NAL Call. No.: RC628.O294 BSB: a new mouse model of multigenic obesity. Fisler, J.S. \u University of California, Los Angeles, CA; Warden, C.H.; Pace, M.J.; Lusis, A.J. Baton Rouge, LA : North American Association for the Study of Obesity, c1993-; 1993 Jul. Obesity research v. 1 (4): p. 271-280; 1993 Jul. Includes references. Language: English Descriptors: Obesity; Multiple genes; Phenotypes; Genetic models; Animal models; Mice 54 NAL Call. No.: QR1.I57 BvgAS-mediated signal transduction: analysis of phase-locked regulatory mutants of Bordetella bronchiseptica in a rabbit model. Cotter, P.A.; Miller, J.F. Washington, D.C., American Society for Microbiology; 1994 Aug. Infection and immunity v. 62 (8): p. 3381-3390; 1994 Aug. Includes references. Language: English Descriptors: Bordetella bronchiseptica; Mutants; Phenotypes; Animal models; Bacterial proteins; Transduction; Strain differences; Virulence; Colonizing ability Abstract: Members of the Bordetella genus alternate between two distinct phenotypic phases in response to changes in their environment. This switch, termed phenotypic modulation, is mediated by the BvgAS sensory transduction system. We developed an animal model based on the interaction of Bordetella bronchiseptica with one of its natural hosts, the rabbit. To investigate the importance of BvgAS signal transduction, we constructed constitutive (RB53) and Bvg- (RB54) phase-locked derivatives of a wild-type strain, RB50. RB50 and RB53, but not RB54, established respiratory infections in B. bronchiseptica-free rabbits with an intranasal 50% infective dose of less than 200 organisms, and the course of the infection closely resembled that observed with naturally infected rabbits. Bacteria were recovered from the nasal cavity, larynx, trachea, and lungs in similar numbers from RB50- and RB53-infected rabbits, yet no pathology was detected by histological examination of lung and tracheal sections. The antibody responses in rabbits inoculated with 50 or RB53 were quantitatively and qualitatively indistinguishable, high titers of antibodies were generated primarily against Bvg+ -phase-specific antigens. No response against flagella, a Bvg- phase factor, was detected. Assessment of bacteria associated with alveolar macrophages indicated that only a small percentage of bacteria, if any, appear to be residing within lung macrophages. We also tested the ability of these strains to survive in a nutrient poor environment, conditions which may be encountered within certain niches in the host or in an environmental reservoir. The Bvg- phase was advantageous for growth under these conditions. Our results indicate the Bvg+ phase is sufficient for establishment of respiratory tract infection in the rabbit and the normal BvgAS-mediated response to environmental signals is not required during initial colonization. The Bvg- phase may play a role at later stages of infection, including persistence, transmission, or survival in the environment. 55 NAL Call. No.: 410.9 P94 Canine models of bone marrow transplantation. Ladiges, W.C.; Storb, R.; Thomas, E.D. Cordova, Tenn. : American Association for Laboratory Animal Science; 1990 Jan. Laboratory animal science v. 40 (1): p. 11-15; 1990 Jan. Includes references. Language: English Descriptors: Dogs; Bone marrow transplant; Models; Human diseases Abstract: Progress in experimental bone marrow transplantation in dogs has provided for the direct transfer of research data to the clinical setting and the therapeutic application of marrow grafting to a variety of human diseases. Animal models of total body irradiation, engraftment and graft-versus-host disease are still needed to solve the existing clinical problems of marrow transplantation. Therefore, work in various canine model systems continues to be of interest. Pet dogs with spontaneously occurring lymphomas are used to study the clinical parameters necessary for applying the technique of transplanting their own marrow (autologous), in conjunction with high dose radiation and/or chemotherapy, to human patients with cancer. A major consideration in the successful transplantation of donor bone marrow (allogeneic) is overcoming histocompatibility barriers to assure engraftment and the prevention of graft-versus-host disease, a major limiting aspect of clinical marrow transplantation. Chemicals, radiation, radiotherapeutic techniques, antisera and monoclonal antibodies have been and continue to be developed in laboratory bred dogs. These approaches suppress the immune system either nonspecifically by ablation of immune reactive tissue, or specifically by affecting certain types of immune reactive cells. Parameters such as clinical effectiveness (engraftment or prevention of graft-versus-host disease), immune reconstitution and undesirable side affects in long-term survivors are all used to determine whether new technology can be transferred from preclinical canine studies to human bone marrow transplantation protocols. 56 NAL Call. No.: 500 N21P Canine X chromosome-linked hereditary nephritis: a genetic model for human X-linked hereditary nephritis resulting from a single base mutation in the gene encoding the alpha-5 chain of collagen type IV. Zheng, K.; Thorner, P.S.; Marrano, P.; Baumal, R.; McInnes, R.R. Washington, D.C. : National Academy of Sciences,; 1994 Apr26. Proceedings of the National Academy of Sciences of the United States of America v. 91 (9): p. 3989-3993; 1994 Apr26. Includes references. Language: English Descriptors: Dogs; Hereditary diseases; Nephritis; Structural genes; Collagen; Mutations; Nucleotide sequences; Exons; Sex linkage; X chromosome; Animal models; Kidneys; Amino acid sequences Abstract: Many families with X-chromosome linked hereditary nephritis (HN) have mutations in the gene on the X chromosome that codes for the alpha5 chain of collagen type IV. Canine X- linked HN is an animal model for human X-linked HN. To study the alpha5(IV) gene in this model, we used the nucleotide sequence published for the human alpha5(IV) cDNA to construct sets of primers covering approximately equal 95% of the complete cDNA. cDNA from both affected and normal dog kidneys was amplified by PCR in nine overlapping regions. The nucleotide sequence encoding the noncollagenous domain NC1 hybridized to the human X chromosome and was 93% identical at the DNA level and 97% identical at the protein level to the human alpha 5(IV) NC1 domain, confirming that the canine alpha 5(IV) cDNA had been amplified. Sequence analysis of the alpha 5(IV) cDNA detected a single nucleotide substitution, G leads to T, in affected dogs, changing a codon for a conserved glycine residue (GGA) to a stop codon (TGA). When genomic DNA was amplified, the same abnormality was found in exon 35. Using the canine NC1 domain cDNA as a probe for Northern analysis, two transcripts of approximately equal to 8.6 kb and approximately equal to 6.7 kb were identified in both normal and affected male dog kidney RNA. However, the abundance of both transcripts was decreased by a factor of approximately equal 10 in the affected dog. These results establish at the molecular level that canine X-linked HN is a model for human X-linked HN. This model provides an opportunity to determine the efficacy of new therapies and to investigate the role of the alpha5(IV) chain in type IV collagen assembly. 57 NAL Call. No.: 442.8 L62 Cardiovascular abnormalities associated with human and rodent obesity. Paulson, D.J.; Tahiliani, A.G. Tarrytown, N.Y. : Pergamon Press Inc; 1992. Life sciences v. 51 (20): p. 1557-1569; 1992. Literature review. Includes references. Language: English Descriptors: Obesity; Diet; Weight reduction; Cardiovascular diseases; Heart; Animal models; Rats; Man; Literature reviews Abstract: Obesity is a major risk factor for cardiovascular disease. However, a direct link between these two states is difficult to establish, since obesity frequently occurs with other disease states such as diabetes, hypertension and atherosclerosis. Clinical studies have clearly shown that uncorrected obesity is associated with cardiac hypertrophy and compromised ventricular function. A number of rodent models of obesity have been studied in terms of cardiovascular adaptations. Cardiac function of the obese Zucker rat appears to be normal at a younger age. Only after several months is depression in cardiac function discernable. These animals are mildly hypertensive, but do not exhibit the characteristic increase in cardiac output associated with human obesity. A unique characteristic of JCR:LA-cp rat is that they develop atherosclerotic and myocardial lesions. Hearts from these animals will maintain normal function when perfused with physiological levels of calcium. At higher calcium concentrations, however, mechanical function becomes impaired. Dietary-induced obese rats exhibit many of the hemodynamic alterations associated with human obesity, but there is no evidence to-date that these animals will develop severe cardiac depression. Short-term weight reduction apparently has beneficial cardiovascular effects, but weight cycling may be harmful. Given the widespread occurrence of obesity, further studies are warranted to characterize the cardiac manifestations of this condition. 58 NAL Call. No.: QP1.C6 Carnitine prolongs the half-life of ethanol in broilers. Smith, M.O.; Cha, Y.S.; Sachan, D.S. Oxford : Pergamon Press Ltd; 1994 Sep. Comparative biochemistry and physiology. A: Comparative physiology v. 109A (1): p. 177-180; 1994 Sep. Includes references. Language: English Descriptors: Ethanol; Metabolism; Carnitine; Supplements; Broilers; Animal models Abstract: The object was to determine if carnitine attenuated ethanol metabolism in broilers similar to that reported in the rats. Two groups (n = 5) of 5-week-old broilers were given for 10 days the feed with or without 0.5% L-carnitine supplement. A single oral dose of ethanol on day 8 was followed by serial blood samples which were analysed for ethanol. Another dose of ethanol was given on day 10 and 2 hr later, plasma and liver were collected and analysed for ethanol, total lipid, triglycerides and carnitine. The carnitine supplemented diet prolonged the half-life of ethanol due to attenuation of ethanol metabolism which is similar to that reported earlier in rodents. The increases in plasma and hepatic acylcarnitines indicate that supplementary carnitine lessens the load of free acyl groups in the liver by eventual oxidation or excretion. 59 NAL Call. No.: 389.8 J82 The carnitine-deprived newborn rabbit: a potential model to study carnitine deficiency. Penn, D.; Schmidt-Sommerfeld, E. Bethesda, Md. : American Institute of Nutrition; 1988 Dec. The Journal of nutrition v. 118 (12): p. 1535-1539; 1988 Dec. Includes 34 references. Language: English Descriptors: Nutrient deficiencies; Carnitine; Neonates; Rabbits Abstract: This report describes the novel development of an animal model for neonatal carnitine deficiency using the artificially fed newborn rabbit. Each litter was separated from the mother following the first colostrum feeding and divided into 2 groups, one of which was fed a purified rabbit formula that was essentially free of carnitine; the other received the same formula supplemented with L-carnitine (100 mg/l). At 9-13 d of age, rabbit pups receiving the carnitine- free formula had lower concentrations of total, free and acylcarnitine in plasma and urine, as well as lower total acid soluble carnitine concentrations in liver, muscle, heart and brown adipose tissue than those receiving the same formula supplemented with L-carnitine. Their plasma and tissue levels were also lower, but their urinary carnitine concentrations were higher than those in naturally-raised pups. The findings suggest that the described animal model may prove to be a useful tool for the investigation of certain aspects of neonatal carnitine deficiency. 60 NAL Call. No.: 389.8 J82 Carotenoids and cancer in animal models. Krinsky, N.I. Bethesda, Md. : American Institute of Nutrition; 1989 Jan. The Journal of nutrition v. 119 (1): p. 123-126; 1989 Jan. Includes references. Language: English Descriptors: Diet; Carotenoids; Carcinoma; Disease prevention Abstract: As evidence accumulated from epidemiological studies that beta-carotene acts as a chemopreventive agent with respect to inhibiting the appearance of certain types of tumors in humans, attention focused on animal models as a means of extending our understanding of carotenoid function. Unfortunately, most animals used in research are "white fat" animals, and require large amounts of carotenoids in their diets to obtain significant blood and tissue levels. Even with these limitations, beta-carotene, a provitamin A carotenoid, as well as canthaxanthin, a nonprovitamin A carotenoid, have been shown to protect animals against UV-induced skin tumors, UV and carcinogen-induced tumors, and carcinogen treatment alone. Similar observations have been made in cell and organ cultures where carotenoids have been shown to prevent malignant transformation and nuclear damage. Although the mechanism of this protection is still unclear, the evidence continues to accumulate that carotenoids may possess intrinsic chemopreventive action with respect to tumor formation. 61 NAL Call. No.: 410.9 P94 Cataracts in a laboratory colony of ferrets. Miller, P.E.; Marlar, A.B.; Dubielzig, R.R. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Dec. Laboratory animal science v. 43 (6): p. 562-568; 1993 Dec. Includes references. Language: English Descriptors: Ferrets; Cataract; Disease prevalence; Histopathology; Animal models; Disease models Abstract: Cataracts were found by use of slit-lamp biomicroscopy in two genetically unrelated ferret populations (A and B). When they were initially examined at the age of 11 to 12 months, 34 of 73 ferrets (46.6%) in population A had lens opacities, which could be categorized into one of three groups. Group-1 ferrets (n = 25) manifested a continuum of lens changes ranging from fine, multifocal, punctate opacification of the superficial posterior lens cortex (n = 3), to changes in both the anterior and posterior cortex (n = 13), to immature (n = 1), or mature/hypermature cataracts (n = 8). Group-2 ferrets (n = 7) had bilateral microphthalmia and cataracts. Group-3 ferrets (n = 2) had minor lens changes involving the nucleus or cortex that were not typical of either group 1 or 2. By the age of 18 months, 41 of the remaining 42 animals in population A had developed fine, multifocal, punctate opacities of the posterior cortex. In group-1 animals, histologic changes in the lens ranged from several 80 X 40-micrometers, punctate, spheroidal lesions in the posterior cortex, to posterior migration of the lens epithelium, Morganian granules, and a complete mature/hypermature cataract. One group-2 ferret had microphthalmia, filling of the lens capsule with a cell-poor, periodic acid-Schiff stain-positive membranous material, and retinal detachment. Population B consisted of 15 adult and 47 6-month-old juvenile ferrets. Eleven adults had multifocal, fine, punctate, posterior cortical opacities, and one adult had a nuclear cataract. Ten juveniles had nuclear cataracts (often in a multifocal punctate pattern); two had fine, multifocal, punctate, posterior cortical opacities; one had multifocal nuclear and posterior cortical opacities; and three had multifocal nuclear opacities that also involved both the anterior and posterior cortices. The ferret may be a potentially useful new animal model for studying mechanisms of cataractogenesis and microphthalmia. Caution should be used when interpreting the ocular toxicity of test compounds in this species. 62 NAL Call. No.: QR188.3.C45 Cellular aspects of autoimmunity. Cruse, Julius M.,_1937-; Lewis, R. E. Basel ; New York : Karger,; 1988. 200 p. : ill. ; 25 cm. (Concepts in immunopathology ; vol. 6). Includes bibliographies and index. Language: English Descriptors: Autoimmunity; Autoimmune diseases; Animal models; Cellular immunity 63 NAL Call. No.: 410.9 P94 Changes in platelet-activating factor, catecholamine, and serotonin concentrations in brain, cerebrospinal fluid, and plasma of pichinde virus-infected guinea pigs. Guo, Z.M.; Qian, C.G.; Peters, C.J.; Liu, C.T. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Dec. Laboratory animal science v. 43 (6): p. 569-574; 1993 Dec. Includes references. Language: English Descriptors: Pichinde virus; Animal models; Epinephrine; Norepinephrine; Immunological factors; Serotonin; Brain; Cerebrospinal fluid; Blood plasma; Physiopathology; Guinea pigs Abstract: Brain concentrations of platelet-activating factor (PAF), catecholamines, and serotonin were measured in control and Pichinde virus-infected strain 13 guinea pigs on postinoculation day (PID) 12. After virus inoculation, PAF concentrations increased 81% in cerebrum, 147% in diencephalon-brain stem, and 110% in cerebellum from baseline values of 2.6 +/- 0.3, 4.3 +/- 0.2, and 6.1 +/- 0.5 (ng/g wet tissue), respectively. Dopamine concentrations in the infected cerebrum and diencephalon-brain stem increased significantly, whereas norepinephrine concentration increased only in cerebrum. However, serotonin concentrations in all three regions of infected brain decreased significantly as compared with control values. There were no significant changes in epinephrine concentrations of infected brain. Norepinephrine and epinephrine concentrations in plasma and cerebrospinal fluid on PID 7 and 12 increased significantly as compared with control values, while plasma dopamine concentration increased significantly on PID 7. Increased brain PAF, dopamine, and norepinephrine concentrations with decreased brain serotonin concentrations may mediate the hyperactivity of the hypothalamic-pituitary-adrenal axis and involve some unknown pathophysiologic processes of arenaviral infection. Furthermore, increased plasma catecholamine concentrations are associated with stress and may be partially responsible for the development of cardiovascular dysfunction and pulmonary edema during this viral disease. 64 NAL Call. No.: 47.8 Am33P Changes in the frequency and size of smooth muscle tumors in Japanese quail lines differing in body weight. Nestor, K.E.; Bacon, W.L. Champaign, IL : Poultry Science Association, 1921-; 1994 Jul. Poultry science v. 73 (7): p. 947-952; 1994 Jul. Includes references. Language: English Descriptors: Japanese quails; Smooth muscle; Neoplasms; Weight; Incidence; Line differences; Body weight; Laying performance; Selection responses; Oviducts; Ligaments Abstract: The purpose of this investigation was to study the incidence and size of smooth muscle tumors in several Japanese quail lines and to report recent correlated changes in mature BW and egg production. Laying females from lines selected solely (HW) or partly (HW-HP; HW-LP) for increased 4-wk BW or for decreased 4-wk BW (LW) and from the corresponding randombred control (R1) were used. Lines HW-HP and HW-LP were sublines of Line HW in which males were selected for increased 4-wk BW and females were selected for high or low level of total plasma phosphorus, respectively. Laying hens were examined for the presence of smooth muscle tumors after about 170 d of egg production (240 d of age). During Generations 19 through 26, mature BW was increasing in the HW line and decreasing in the LW line. Selection for either increased or decreased 4-wk BW resulted in decreased egg production, but the only significant change with generations was a decrease of 2.7 eggs per hen for a 120-d laying period in the LW line. Frequency and weight of the smooth muscle tumors were greater for females from the large-bodied lines than females from Line R1. No tumors were detected in LW females. Based on the linear regression of response on generations, tumor frequency was increasing in Line HW-LP but tumor weight was decreasing in this line. Tumor weight was increasing in the HW line. No other changes in tumor frequency or size were noted across generations. Weight of the tumors was not correlated with egg production. The presence of tumors did not seem to affect mortality during the laying period. The Japanese quail lines may serve as a useful animal model for the study of smooth muscle tumors in humans, chickens, and turkeys. 65 NAL Call. No.: SF95.A1C6 The changing role of animal models in human nutrition research. West, C.E.; Beynen, A.C. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 1-13; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Literature review. Includes references. Language: English Descriptors: Laboratory animals; Animal models; Nutrition physiology; Human nutrition research; Vitamins; Nutrient requirements; Species differences; Literature reviews 66 NAL Call. No.: QL55.A1L3 Characteristics of mutant mice (ICGN) with spontaneous renal lesions: a new model for human nephrotic syndrome. Ogura, A.; Asano, T.; Matsuda, J.; Takano, K; Nakagwa, M.; Fukui, M. London : Royal Society of Medicine Services; 1989 Apr. Laboratory animals v. 23 (2): p. 169-174. ill; 1989 Apr. Includes references. Language: English Descriptors: Mice; Mutants; Disease models; Nephrotic syndrome; Glomerulonephritis; Histopathology Abstract: Spontaneous nephrotic mice (ICGN mice), a new mutant strain of mouse from outbred ICR, were clinically, macroscopically, histologically and immunohistochemically studies to establish their value as a model for human nephrotic syndrome. Most of the affected mice developed proteinuria, hypoproteinaemia and hypercholesterolaemia, and some of them developed systemic oedema. A high concentration of blood urea nitrogen (BUN) and a low haematocrit value were also observed. The kidneys of severe cases showed a decrease in size and had a yellowish granular surface. These findings indicated that the mice were terminally affected by chronic of renal insufficiency. Histopathology demonstrated glomerular lesions consisting of thickened basement membranes of the capillary loops with irregular spike-like protrusions and enlargement of the mesangium unaccompanied by cellular proliferation. The immunofluorescence technique revealed positive granular staining for IgA, IgG and IgM and to a lesser extent for C3 along the capillary loops in affected mice. The similarity between this spontaneous disease and human nephrotic syndrome caused by idiopathic glomerular lesions is discussed. ICGN mice may be a useful animal model for this human disease. 67 NAL Call. No.: QL55.A1L3 Characterization of acute and latent herpes simplex virus infection of dorsal root ganglia in rats. Blondeau, J.M.; Aoki, F.Y.; Glavin, G.B.; Nagy, J.I. London : Royal Society of Medicine Services; 1991 Apr. Laboratory animals v. 25 (2): p. 97-105; 1991 Apr. Includes references. Language: English Descriptors: Rats; Herpes simplex virus; Ganglia; Acute infections; Latent infections; Animal models; Experimental infections; Subcutaneous injection; Feet Abstract: The characteristics of HSV type-1 infection following subcutaneous inoculation in the dorsum of one hind paw of Sprague-Dawley rats were studied to determine whether infection in rats might more closely parallel the infection in man than is seen in other animals. The serologic and virologic characteristics of acute and latent ganglion infection conformed to those of human infection. Immunohistochemical studies suggested that sensory ganglion infection arose via centripetal axonal migration of virus as is hypothesized in man. In rat, small type B neuronal cell bodies appeared central to the maintenance of latent infection and reactivation observed during cocultivation of lumbar ganglia. Acute and latent lumbar sensory ganglion infection in rats after subcutaneous hind paw injection of HSV-1 appears to be another suitable model of this infection in man. 68 NAL Call. No.: 41.8 J82 Chediak-Higashi syndrome in rats: light and electron microscopical characterization of abnormal granules in beige rats. Ozaki, K.; Maeda, H.; Nishikawa, T.; Nishimura, M.; Narama, I. London : Academic Press; 1994 May. Journal of comparative pathology v. 110 (4): p. 369-379; 1994 May. Includes references. Language: English Descriptors: Chediak-higashi syndrome; Histopathology; Cell ultrastructure; Granules; Rats; Animal models 69 NAL Call. No.: QL55.A1L3 Chest roentgenographic techniques for demonstrating human lung tumour xenografts in nude rats. Zeligman, B.E.; Howard, R.B.; Marcell, T.; Chu, H.; Rossi, R.P.; Mulvin, D.; Johnston, M.R. London : Royal Society of Medicine Services; 1992 Apr. Laboratory animals v. 26 (2): p. 100-106; 1992 Apr. Includes references. Language: English Descriptors: Rats; Animal models; Disease models; Neoplasms; Lungs; Radiography; Monitoring Abstract: Roentgenographic techniques were investigated for imaging orthotopic tung tumours in anaesthetized nude rats endobronchially implanted with human lung cancer cells. A conventional radiographic unit with a dual-screen, double- emulsion film mammographic receptor produced images preferable to those from a mammographic unit because of superior resolution. Typical exposure factors were 300 mA, 29 kVp, and 17 ms at a focus-film distance of 76 cm with a 2.11 by 2.41 mm effective focal spot and inherent filtration of 1.2 mm aluminium. Sensitivity for tumour detection was 0.93 for 59 animals with pathologically proved tumours and 0.96 for 54 animals with tumours larger than 4 mm or 50 mg. For 24 pathologically tumour-free animals, specificity was 1-00. For 55 animals radiographically judged to have tumours, positive predictive value was 1.00. For all 83 animals, accuracy was 0.95. This technique effectively demonstrates orthotopic human lung tumours in nude rats and should be useful for noninvasive monitoring of tumour presence, location, size, and changes in size. 70 NAL Call. No.: 47.8 B77 Chicken neoplasia--a model for cancer research. Calnek, B.W. Oxfordshire : Carfax Publishing Company; 1992 Mar. British poultry science v. 33 (1): p. 3-16; 1992 Mar. Literature review. Includes references. Language: English Descriptors: Fowls; Neoplasms; Animal models 71 NAL Call. No.: RA1190.A7 Chlorpyrifos-induced delayed polyneuropathy. Capodicasa, E.; Scapellato, M.L.; Moretto, A.; Caroldi, S.; Lotti, M. Berlin, W. Ger. : Springer; 1991. Archives of toxicology v. 65 (2): p. 150-155; 1991. Paper presented at the International Symposium on "Biochemical and Cellular Indices of Toxicity in Occupational and Environmental Medicine," June 1986, Milan, Italy, at a meeting held March 1986, New Orleans, LA, and at a meeting held Aug/Sept 1989, Praglia, Italy. Includes references. Language: English Descriptors: Chlorpyrifos; Nervous system diseases; Neurotoxins; Acetylcholinesterase; Esterases; Pharmacokinetics; Brain; Man; Fowls; Hens Abstract: Chlorpyrifos [0,0-diethyl 0-(3,5,6-trichloro- pyridyl) phosphorothioate] caused delayed polyneuropathy in man. Contrary to previous studies, we report here that it also causes delayed polyneuropathy in the hen, the animal model for this toxicity. The minimal neuropathic dose was 60-90 mg/kg p.o., corresponding to 4-6 times the estimated LD50. Consequently, pralidoxime (2-PAM) in conjunction with atropine was necessary to reverse acetylcholinesterase AChE) inhibition and cholinergic toxicity in hens given high enough doses of chlorpyrifos to cause neuropathy. Chlorpyrifos was slowly absorbed after single oral doses and the threshold of inhibition (>70%) of neuropathy target esterase (NTE), the putative target for delayed neuropathy, was reached within 5-6 days. High AChE inhibition (>90%), however, was measured within hours after dosing because of the higher potency of chlorpyrifos to inhibit this enzyme. In vitro studies showed that chlorpyrifos-oxon, the active metabolite of chlorpyrifos, was 10-20 times more active against AChE than against NTE, confirming the clinical observation. No differences were seen between human and hen enzymes in this respect. Hen and human brain homogenates contain A-esterases which hydrolysed chlorpyrifos to about the same extent in both species. In conclusion, chlorpyrifos causes delayed polyneuropathy in the hen, as was reported in man. The reasons for previous negative data in the hen are probably due to the relatively lower doses which were used. Judging from in vitro studies with hen and human enzymes, there are no differences in the two species as far as their relative sensitivity to delayed polyneuropathy. It is likely that delayed polyneuropathy would develop in both species only after severe cholinergic toxicity requiring aggressive antidotal treatment. 72 NAL Call. No.: 389.8 B773 The cholesterol-raising effect of coffee in the Syrian hamster. Sanders, T.A.B.; Sandaradura, S. Cambridge : Cambridge University Press; 1992 Sep. The British journal of nutrition v. 68 (2): p. 431-434; 1992 Sep. Includes references. Language: English Descriptors: Diet; Coffee; Blood plasma; Cholesterol; Hamsters Abstract: Adult male Syrian hamsters were fed on a high-fat diet with or without access to boiled coffee. Plasma total, low-density-lipoprotein- and high-density-lipoprotein- cholesterol and triacylglycerol concentrations were increased by the coffee and very-low-density-lipoprotein-cholesterol concentrations were lowered. It is concluded that the Syrian hamster is a suitable animal model in which to study the hypercholesterolaemic effect of coffee. 73 NAL Call. No.: QH301.N32 Chronic alcoholism, malnutrition, and folate deficiency. Halsted, C.H. New York, N.Y. : Plenum Press; 1991. NATO ASI series : Series A : Life sciences v. 206: p. 237-251; 1991. In the series analytic: Alcoholism a molecular perspective / edited by T.N. Palmer. Literature review. Includes references. Language: English Descriptors: Alcoholism; Chronic course; Deficiency diseases; Folic acid; Malabsorption; Malnutrition; Metabolism; Physiopathology; Veterans; Animal models; Literature reviews 74 NAL Call. No.: SF601.A5 Clinical evaluation of cyclosporine in animal models with cutaneous immune-mediated disease and epitheliotropic lymphoma. Rosenkrantz, W.S.; Griffin, C.E.; Barr, R.J. Golden, Colo. : The Association; 1989 Jul. The Journal of the American Animal Hospital Association v. 25 (4): p. 377-384. ill; 1989 Jul. Includes references. Language: English Descriptors: Dogs; Cat; Epithelium; Lymphoma; Treatment; Immunological diseases; Drug therapy; Immunosuppressive agents 75 NAL Call. No.: QP141.A1A63 Cobalamin deficiency and the pathogenesis of nervous system disease. Metz, J. Palo Alto, Calif. : Annual Reviews, Inc; 1992. Annual review of nutrition v. 12: p. 59-79. ill; 1992. Literature review. Includes references. Language: English Descriptors: Vitamin b12; Vitamin deficiencies; Demyelination; Animal models; Nitrous oxide; Biochemistry; Methylation; Toxicity; Literature reviews 76 NAL Call. No.: RA421.P684 Colon cancer: dietary modifications required for a balanced protective diet. McIntosh, G.H. Orlando, Fla. : Academic Press; 1993 Sep. Preventive medicine v. 22 (5): p. 767-774; 1993 Sep. Paper presented at the Fourth International Conference on Prevention of Human Cancer: Nutrition and Chemoprevention Controversies, June 3-6, 1992, Tucson, Arizona. Includes references. Language: English Descriptors: Carcinoma; Colon; Disease prevention; Diet; Animal models; Fiber; Dietary protein; Dietary fat; Vitamin e; Calcium; Nutrient nutrient interactions; Animal fat; Animal protein; Rats Abstract: Background. There is increasing support of the view that our diet is too calorie dense, with its high animal fat, sugar, and alcohol content. Food processing has helped to create this situation as well as the desire to eat sugar- and fat-rich foods. By examining the influence of these dietary effects on colon cancer, experimental animal studies can help dissect the influences not readily assessable by epidemiological means. Methods. The Sprague Dawley rat model of colon cancer induced by dimethylhydrazine provides a means of assessing dietary influences with the use of a semipurified diet and varying a single factor at a time. We have examined the influence of Ca vitamin E, protein type, and cereal dietary fiber sources on tumor burden and incidence in rats on a standardized experimental protocol. Results. A significant interactive effect has been seen with high Ca and low vitamin E intake in protecting rats from tumors. When comparing differing protein sources, whey protein concentrate was found to be very protective relative to red meat and other protein sources. Spent barley grain was also shown to be very protective relative to wheat bran and commercial barley bran. Conclusions. There are several potentially useful strategies for protection from colon cancer by varying diet composition. Protein sources such as whey protein concentrate, insoluble dietary fiber from barley grain, and high calcium intake seem to be very promising. These need further detailed examination as to whether they can combine to reduce risk further and to understand better the mechanisms responsible for protection. They may provide greater potential than attempts to lower the fat in the human diet. 77 NAL Call. No.: QR180.C62 Comparative features of retroviral infections of livestock. Evermann, J.F. Exeter : Pergamon Press; 1990. Comparative immunology, microbiology and infectious diseases v. 13 (3): p. 127-136; 1990. Literature review. Includes references. Language: English Descriptors: Livestock; Man; Lentivirinae; Oncovirinae; Disease transmission; Spread; Pathogenesis; Host specificity; Viral diseases; Disease models; Literature reviews; Animal models Abstract: Retrovial infections of livestock have become of increasing importance due to their usefulness as comparative models for human retroviral infections and their effects upon animal health and marketability of animals and animal products nationally and internationally. This paper presents a perspective on the retroviruses of economic concern in veterinary medicine with emphasis on the importance of understanding the modes of virus transmission and the species specificity of the viruses. The retroviruses reviewed include the oncovirus, bovine leukosis virus, and the lentiviruses, equine infectious anemia virus; maedi/visna virus, caprine arthritis-encephalitis virus and bovine visna-like virus. The comparative features amongst these animal retroviruses and those of humans must be recognized by the veterinary and medical professions since the similarities in virus replication and spread by blood transfer can provide important clues in controlling and perhaps preventing human retroviruses infections, such as the human immunodeficiency virus. 78 NAL Call. No.: 41.8 AM3A Comparative virulence of Haemophilus parasuis serovars 1 to 7 in guinea pigs. Rapp-Gabrielson, V.J.; Gabrielson, D.A.; Schamber, G.J. Schaumburg, Ill. : American Veterinary Medical Association; 1992 Jun. American journal of veterinary research v. 53 (6): p. 987-994; 1992 Jun. Includes references. Language: English Descriptors: Haemophilus; Virulence; Serotypes; Strain differences; Guinea pigs; Intraperitoneal injection; Application methods; Morbidity; Mortality; Disease models Abstract: Reference strains for Haemophilus parasuis serovars 1 to 7 were examined for virulence by inoculation of guinea pigs. Guinea pig response to intraperitoneal inoculation was similar for the 7 reference strains. However, apparent differences in virulence were detected after intratracheal inoculation. Cells of the reference strains for serovars 1 and 5 were most invasive, causing moribundity or death at higher doses and a persistent septicemia at lower doses. Haemophilus parasuis could be isolated from respiratory and systemic sites; purulent bronchopneumonia, pericarditis, and pleuritis were apparent in infected guinea pigs. Inoculation of cells of the reference strains for serovars 2 and 6 also resulted in bronchopneumonia and moribundity or death in some guinea pigs; however, reisolation of H parasuis and microscopic lesions at necropsy were less pronounced than those observed with serovars 1 and 5. Inoculation of cells of serovars 3, 4, and 7 induced only transient clinical signs and minimal evidence of H parasuis infection at necropsy. The data from intratracheal inoculation of guinea pigs are similar to data from other investigations in swine, indicating differences in the pathogenic potential of H parasuis strains. Thus, guinea pigs may be useful as a laboratory animal model for examining cellular factors associated with virulence and immunogenicity of H parasuis. 79 NAL Call. No.: 410.9 P94 Comparison of hematologic parameters in normal and streptozotocin-induced diabetic rats. Alder, V.A.; Yu, D.Y.; Su, E.N.; Cringle, S.J. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Apr. Laboratory animal science v. 42 (2): p. 170-173; 1992 Apr. Includes references. Language: English Descriptors: Rats; Diabetes; Animal models; Hematology; Normal values; Blood sugar; Hemoglobin; Glycerate 2,3-bis(phosphate) Abstract: Hematologic values are compared for normal and streptozotocin-induced diabetic rats after 6 weeks of induced diabetes. Most hematologic parameters were the same in the two groups except for blood glucose, glycated hemoglobin, and 2,3 diphosphoglycerate, all of which were elevated in the streptozotocin group. However the P50 (the P02 at which the oxygen-carrying capacity of blood is 50% of maximal) remained normal. We hypothesize that a left shift in the oxyhemoglobin dissociation curve caused by the glycation of a small percentage of the hemoglobin is compensated by elevation in the 2,3-diphosphoglycerate which returns the P50 to normal values. This compensatory mechanism also occurs in some stages of human diabetes. 80 NAL Call. No.: QP141.A1N88 Comparison of the effect of dietary casein and cottonseed protein on food intake and growth in normal tumor-bearing rats. Radcliffe, J.D. Elmsford, N.Y. : Pergamon Press; 1991 Sep. Nutrition research v. 11 (9): p. 1055-1066; 1991 Sep. Includes references. Language: English Descriptors: Dietary protein; Casein; Cottonseed protein; Food intake; Growth rate; Neoplasms; Rats Abstract: Male Fischer 344 rats with (tumor-bearers) and without (controls) a transplantable methylcholanthrene sarcoma were fed isonitrogenous, isoenergetic diets containing either casein or cottonseed protein (CSP) so as to compare the effects of these two proteins on the development of cancer- induced anorexia and cachexia. For both diets, tumor growth was associated with depressed food intake, decreased body weight, hypoalbuminemia and hyperlipidemia. Diet had no effect on food intake, weight gain or serum albumin for either controls or tumor-bearers; tumor weight was unaffected by type of dietary protein. Liver weights were lower for animals fed CSP than for those fed casein. Dietary CSP exerted a hypolipidemic effect in normal rats, but this differential effect of protein quality on serum lipids was abolished by tumor growth, as were differences in serum fatty acid profile associated with consumption of CSP. Tumor growth itself was associated with altered fatty acid profiles in serum, with the percentages of fatty acids as stearic and arachidonic acids being decreased and the percentages as oleic and linoleic acids being increased. Thus, dietary CSP has similar effects to casein on the development of cancer anorexia and cachexia in this animal model. The effects of protein quality on serum lipids, however, can be altered by tumor growth. 81 NAL Call. No.: SF757.8.A4 Computed tomography of rambouillet sheep affected with neuronal ceroid lepofuscinosis. Woods, P.R.; Walker, M.A.; Weir, V.A.; Storts, R.W.; Menzies, C.; Shelton, M. Raleigh, NC : American College of Veterinary Radiology; 1994 Jul. Veterinary radiology & ultrasound : the official journal of the American College of Veterinary Radiology and the International Veterinary Radiology Association v. 34 (4): p. 259-262; 1994 Jul. Includes references. Language: English Descriptors: Sheep; Computed tomography; Neurons; Degeneration; Brain; Ceroid; Thalamus; Diagnosis; Postmortem examinations; Animal models 82 NAL Call. No.: QL55.A1I43 The contribution of nonhuman primates to understanding coronary artery atherosclerosis in humans. Clarkson, R.B.; Klumpp, S.A. Washington, D.C. : Institute of Laboratory Animal Resources, National Research Council; 1990. I.L.A.R. news v. 32 (2): p. 4-8; 1990. Includes references. Language: English Descriptors: Monkeys; Animal models; Disease models; Atherosclerosis; Cholesterol; Blood plasma; Tobacco smoking; Stress; Sex differences; Oral contraceptives 83 NAL Call. No.: RC620.A1N47 Control of hypoallergenicity by animal models. Pahud, J.J.; Schwarz, K.; Granato, D. New York, N.Y. : Raven Press; 1988. Nestle nutrition workshop series v. 17: p. 199-207; 1988. Includes references. Language: English Descriptors: Food allergies; Immune response; Allergens; Hypersensitivity; Models; Breast feeding 84 NAL Call. No.: RA421.P684 Controversial issues of dietary fat and experimental mammary carcinogenesis. Ip, C. Orlando, Fla. : Academic Press; 1993 Sep. Preventive medicine v. 22 (5): p. 728-737; 1993 Sep. Paper presented at the Fourth International Conference on Prevention of Human Cancer: Nutrition and Chemoprevention Controversies, June 3-6, 1992, Tucson, Arizona. Includes references. Language: English Descriptors: Mammary gland neoplasms; Dietary fat; Linoleic acid; Diet; Caloric intake; Risk; Pregnancy; Lactation; Carcinogenesis; Literature reviews Abstract: Epidemiological evidence from different countries worldwide has suggested a positive association between the availability of fat in the diet and variations in breast cancer mortality rate. A voluminous amount of information is also available in the literature linking increased fat consumption, particularly polyunsaturated fat, and stimulation of mammary tumorigenesis in animal models. In the past few years, our laboratory has been studying the impact of several confounding factors that could modulate the enhancing effect of fat on neoplastic development of the mammary gland in female rats which are treated with a carcinogen. It is our conclusion that fat promotes mammary carcinogenesis only under a very stringent set of conditions which might not be duplicated in the arena of fat intake and human breast cancer risk. Previous studies on fat and mammary cancer in experimental models have used young virgin rats which are given a dose of carcinogen at a particular age. The question arises as to whether the promoting effect of fat might be a consequence of the characteristics of the model. We have supportive evidence showing that the following criteria must be satisfied in order for fat enhancement of mammary carcinogenesis to be manifested: (a) carcinogen administered at a time when the mammary gland is exquisitely susceptible to tumor induction, (b) animals maintained on a semipurified diet, (c) ad libitum feeding necessary, and (d) unusually high requirement of linoleic acid for tumor development. On the other hand, the stimulatory effect of fat is attenuated or sometimes even negated by (a) feeding of a natural ingredient diet, (b) submaximal calorie intake, and (c) previous history of pregnancy and lactation. Given the spectrum of confounders that are inherent in epidemiological studies linking fat intake and breast cancer, including differences in lifestyle, reproductive history, eating habits, as well as complexity of the total diet, our findings suggest that there may be a need to reevaluate the validity of extrapolating animal data that are obtained under a highly defined set of conditions to the etiological significance of dietary fat in human breast cancer. 85 NAL Call. No.: 410.9 P94 Convulsions in senescence-accelerated mice (SAM-R/1/Eis). Yamazaki, K.; Kumazawa, A.; Ito, K.; Kurihara, K.; Nakayama, M.; Wakabayashi, T. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Aug. Laboratory animal science v. 42 (4): p. 378-381; 1992 Aug. Includes references. Language: English Descriptors: Mice; Animal models; Convulsions; Aging Abstract: Senescence-accelerated mice (SAM) are one of the animal models used for studying senescence, which consist of several substrains such as SAM-R/1, R/2, P/1, P/2. SAM-R/1/Eis maintained in Eisai Tsukuba Research Laboratories, Ibaraki, Japan, was originally introduced as a substrain of a normal control SAM-R/1 from Kyoto University, Japan. We have noted signs of convulsions in SAM-R/1/Eis mice during routine animal care, particularly while changing cages. We identified the clinical signs and determined the concentrations of glucose and immunoreactive insulin in plasma of SAM-R/1/Eis mice. There were no differences in the male:female ratios of mice showing prodrome only, grand mal, or no-signs. The ages at which prodrome and grand mal were first noted peaked between 20 and 25 weeks. Concentrations of glucose and immunoreactive insulin in plasma did not indicate the mice were in insulin hypoglycemia, which is one cause of convulsions. AKR strain mice, some of which originated with the SAM strain are known to become convulsive by repeated "throwing" stimulations. Conversely, in SAM-R/1/Eis, throwing stimuli are not needed to cause convulsive signs. Thus it is likely that in SAM-R/1/Eis mice the signs are triggered by repeating mild environmental changes, such as changing cages. The results of this study show that SAM-R/1/Eis is neither a normal control strain, nor an original SAM-R/1 strain. But it is possible that SAM- R/1/Eis is another useful animal model for studying spontaneous convulsion. 86 NAL Call. No.: 410.9 P94 Coronary arterial abnormalities in hyperlipidemic rats with renal failure. Yamasaki, K.; Yoshikawa, Y. Cordova, Tenn. : American Association for Laboratory Animal Science; 1994 Apr. Laboratory animal science v. 44 (2): p. 125-130; 1994 Apr. Includes references. Language: English Descriptors: Rats; Hyperlipemia; Renal failure; Coronary vessels; Arteries; Disease course; Heart; Kidneys; Histopathology; Cholesterol; Triacylglycerols; Phospholipids; Urea; Nitrogen; Blood pressure; Weight Abstract: Hyperlipidemic rats, which have been described as a useful animal model for focal glomerulosclerosis in humans, were examined at the ages of 17, 20, 24, and 27 weeks for evaluation of spontaneously developed coronary arterial lesions. The mean concentrations of cholesterol, triglyceride, phospholipid, and urea nitrogen were greater than the respective control concentrations at and after the age of 17 weeks. No abnormalities were detected in the blood pressure values. Starting from the age of 24 weeks, the rats had disseminated white spots in the ventricles and septum of the heart. Mean renal weights of hyperlipidemic rats were higher than those of control rats at the ages of 17 and 20 weeks, and the surface of the kidney appeared irregular when rats were 27 weeks old. Histologic examination revealed atrophy of the coronary artery, a decrease in the number of smooth muscle cells, and thinning of the wall, resulting in loss of the normal wall structure. A homogenous eosinophilic substance, the nature and cause of which were unknown, was also seen in the affected arterial walls. Furthermore, white spots observed macroscopically were found to represent myocardial degeneration and necrosis with reactive histiocytic cells and lymphocytes, adventitial fibrosis, and edema associated with the affected arteries. These arterial lesions became evident in rats at and after the age of 24 weeks. Electron microscopic examination of coronary arteries revealed enlargement of the subendothelial space and spaces between the smooth muscle cells containing cell debris in rats at the age of 20 weeks, and degeneration and necrosis of the endothelial cells, smooth muscle cells in the media, and striated muscle cells adjacent to the affected arteries in rats at the age of 27 weeks. Histologic examination of affected kidneys revealed focal glomerulosclerosis, accompanied by the dilatation of the tubules, which contained eosinophilic casts and infiltrating lymphocytes in the interstitium together with edema, at and after the age of 17 weeks. 87 NAL Call. No.: RC927.C73 CRC handbook of animal models for the rheumatic diseases.. Handbook of animal models for the rheumatic diseases Greenwald, Robert A.,_1943-; Diamond, Herbert S., Boca Raton, Fla. : CRC Press,; 1988. 2 v. : ill. ; 26 cm. Includes bibliographies and index. Language: English Descriptors: Rheumatism; Animal models; Handbooks, manuals, etc; Arthritis; Animal models; Handbooks, manuals, etc; Animal welfare 88 NAL Call. No.: RC756.H28 CRC handbook of animal models of pulmonary disease.. Handbook of animal models of pulmonary disease Cantor, Jerome O. Boca Raton, Fla. : CRC Press,; 1989. 2 v. : ill. ; 26 cm. Includes bibliographies and indexes. Language: English Descriptors: Lungs 89 NAL Call. No.: 381 J824 Defective glucose-dependent endoplasmic reticulum Ca2+ sequestration in diabetic mouse islets of Langerhans. Roe, M.W.; Philipson, L.H.; Frangakis, C.J.; Kuznetsov, A.; Mertz, R.J.; Lancaster, M.E.; Spencer, B.; Worley, J.F. III; Dukes, I.D. Bethesda, Md. : American Society for Biochemistry and Molecular Biology; 1994 Jul15. The Journal of biological chemistry v. 269 (28): p. 18279-18282; 1994 Jul15. Includes references. Language: English Descriptors: Mice; Experimental diabetes; Diabetes mellitus; Calcium ions; Endoplasmic reticulum; Glucose; Pyrophosphatases; Enzyme activity; Pancreas islets; Insulin secretion Abstract: Non-insulin-dependent diabetes mellitus (NIDDM) is a metabolic disease associated with abnormal insulin secretion, the underlying mechanisms of which are unknown. Glucose-dependent signal transduction pathways were investigated in pancreatic islets derived from the db/db mouse, an animal model of NIDDM. After stimulation with glucose (4-12 mM), the changes in intracellular Ca2+ concentration (Ca2+]i) were different; unlike control islets, db/db islets lacked an initial reduction of [Ca2+]i and the subsequent [Ca2]i oscillations following stimulation with 12 mM glucose. The severity of these defects in Ca2+ signaling correlated with the age-dependent development of hyperglycemia. Similarly defective glucose-induced Ca2+ signaling were reproduced in control islets by pre-exposure to thapsigargin, a selective inhibitor of endoplasmic reticulum (ER) Ca2+-ATPase. Estimation of ATPase activities from rates of ATP hydrolysis and by immunoblot hybridization with an antiserum directed against the sacro/endoplasmic reticulum Ca2+-ATPase both demonstrated that the ER Ca2+-ATPase was almost entirely absent from db/db islets. The effects of inhibition of ER Ca2+-ATPase on insulin secretion were also examined; a 4-day exposure of control islets to 1 micromolar thapsigargin resulted in basal and glucose-stimulated insulin secretion levels similar to those found in db/db islets. These results suggest that aberrant ER Ca2+ sequestration underlies the impaired glucose responses in the db/db mouse and may play a role in defective insulin secretion associated with NIDDM. 90 NAL Call. No.: 41.8 V643 The development of a vaccine against feline immunodeficiency virus. Hosie, M.J. London : Bailliere Tindall; 1994 Jan. The British veterinary journal v. 150 (1): p. 25-39; 1994 Jan. Includes references. Language: English Descriptors: Cats; Vaccines; Feline immunodeficiency virus; Infection; Vaccine development; Vaccination; Disease prevention; Literature reviews Abstract: Feline immunodeficiency virus (FIV) is a retrovirus causing significant disease in cats. The virus has been shown to be similar biologically to the human immunodeficiency virus (HIV), the cause of acquired immunodeficiency syndrome (AIDS) in humans. Much interest has been expressed in the use of FIV as an animal model for HIV vaccination studies. Both FIV and HIV belong to the lentivirus group of retroviruses. While there are several effective vaccines against feline leukaemia virus (FeLV), a mammalian type C retrovirus, at present there are no effective vaccines against lentiviruses. This review illustrates the obstacles to the production of vaccines against FIV or HIV. FIV vaccine studies conducted in several laboratories are reviewed, the results are compared and factors important for inducing protection from FIV infection are discussed. 91 NAL Call. No.: RC628.O22 Development of insulin resistance during the course of obesity: lessons from animal models. Penicaud, L.; Ferre, P. New York, N.Y. : Human Sciences Press; 1988. Journal of obesity and weight regulation v. 7 (2): p. 91-109; 1988. Literature review. Includes references. Language: English Descriptors: Diabetes; Obesity; Insulin; Adipose tissue; Glucose tolerance; Animal models; Genetic markers; Experimental diets; Hypothalamic lesions; Metabolism; Lipids; Literature reviews; Rats 92 NAL Call. No.: RC628.N48 1987 The development of the SHR/N- and LA/N-cp (Corpulent) congenic rat strains. Hansen, C.T. Bethesda, Md. : National Institutes of Health; 1988. New models of genetically obese rats for studies in diabetes, heart disease, and complications of obesity : NIH workshop, June 18-19, 1987, summaries of workshop papers and current bibliography. p. 7-11; 1988. Language: English Descriptors: Obesity; Animal breeding; Animal models; Rats 93 NAL Call. No.: 381 J8282 Development of unesterified cholesterol-rich lipid particles in atherosclerotic lesions of WHHL and cholesterol-fed NZW rabbits. Chao, F.F.; Blanchette-Mackie, E.J.; Dickens, B.F.; Gamble, W.; Kruth, H.S. Bethesda, Md. : Lipid Research, inc., 1959-; 1994 Jan. Journal of lipid research v. 35 (1): p. 71-83; 1994 Jan. Includes references. Language: English Descriptors: Rabbits; Experimental atherosclerosis; Cholesterol; Lipids; Animal models; Disease models; Hyperlipemia; Phosphatidylcholines; Sphingomyelins Abstract: Previously, we isolated and characterized unesterified cholesterol-rich lipid particles (UCLP) that accumulate in extracellular spaces of atherosclerotic lesions of humans and cholesterol-fed rabbits. In the present study, we examined early developing atherosclerotic lesions to determine when UCLP appear and when they become enriched in cholesterol and sphingomyelin. Cholesterol-fed NZW rabbits, which rapidly develop atherosclerotic lesions, and genetically hyperlipidemic WHHL rabbits, which develop lesions over a longer period of time, were studied. UCLP of peak density 1.04 g/ml appear as early as 4 weeks after the onset of cholesterol feeding and progressively accumulate during atherosclerotic lesion development. Beginning with their appearance and afterwards, UCLP contain a saturating level (2:1 molar ratio) of cholesterol relative to phospholipid. Whereas, early UCLP are enriched in phosphatidylcholine, with time UCLP become enriched with sphingoymelin. Another UCLP population having a peak density of 1.09 g/ml was present in control aortas and increased in amount more slowly than the d 1.04 g/ml UCLP during cholesterol feeding. The d 1.09 g/ml particles were predominantly unilamellar vesicles, the majority between 100 and 200 nm in diameter. They contained > 90% of their cholesterol in unesterified form and their ratio of unesterified cholesterol to phospholipid progressively increased from 0.6 to 1.7 during cholesterol feeding. Liposome resistance to solubilization by high density lipoproteins is known to be increased by enrichment with unesterified cholesterol and sphingomyelin. Sphingomyelin enrichment of unesterified cholesterol-rich lipid particles (UCLP) could stabilize cholesterol in a form that does not readily crystallize. However, at the same time, the early and progressive accumulation of UCLP in developing atherosclerotic lesions may limit reverse cholesterol transport and accelerate disease progression. 94 NAL Call. No.: QP501.E8 Developmental changes of 6-phosphofructo-1-kinase subunit levels in erythrocytes from normal dogs and dogs affected by glycogen storage disease type VII. Mhaskar, Y.; Harvey, J.W.; Dunaway, G.A. New York, NY : Springer-Verlag New York Inc; 1992 Mar. European journal of biochemistry v. 101 (3): p. 303-307; 1992 Mar. Includes references. Language: English Descriptors: Dogs; Glycogenosis; Phosphofructokinase; Isoenzymes; Enzyme activity; Erythrocytes; Age differences; Animal models Abstract: 1. The subunit proportions (L:M:C) of the PFK isozymes from normal adult erythrocytes were 2:86:12. Affected adult erythrocyte 6-phosphofructo-1-kinase (PFK) isozymes contained normal L-type (31%) and C-type (61%) subunits as well as a small amount (8%) of truncated M-type subunit. 2. When measured within 24 hr of birth, both normal and affected dog erythrocytes contained high PFK activities due to elevated levels of the L-type subunit. As the dogs matured, PFK activity decreased due to a greater than 99% loss of the L- type subunit. 3. By 2 weeks of age, the M-type and C-type subunits in normal dog PFK isozymes increased severalfold and attained near adult levels. 4. During post-natal development, the L-type subunit from affected dog erythrocytes decreased more rapidly than from normal dog erythrocytes; but it was maintained at a higher level in the affected adult erythrocytes. Also, in the affected dog erythrocytes, truncated M-type subunits were detected; and the initially high levels of the C-type subunit decreased approximately 50% after 4 weeks. 95 NAL Call. No.: QP141.A1P72 Diabetes mellitus. What have we learned from animals?. Berdanier, C.D. Tarrytown, N.Y. : Pergamon Press; 1993 Jul. Progress in food & nutrition science v. 17 (3): p. 261-285; 1993 Jul. Includes references. Language: English Descriptors: Diabetes mellitus; Animal models; Animal experiments; Insulin; Obesity; Incidence; Pancreas islets; Autoimmune diseases; Viral diseases; Blood sugar; Glucose; Nutrient transport; Carbohydrate metabolism; Literature reviews Abstract: Progress in our understanding of the pathophysiology of diabetes mellitus has been made possible because of the availability of animal analogs of the various human diseases. Diabetes mellitus can be mild, moderate or severe depending on the genetic error that is responsible for the disease. Present estimates of errors that result in diabetes range from 20 to 100. Because similar errors have been found in spontaneously diabetic animals scientists have been able to identify the sequence of metabolic events and subsequent tissue change in many of these phenotypes. Studies of the efficacy of various drugs, diets and lifestyle choices on disease development and management thus were made possible. 96 NAL Call. No.: QL55.A1I43 Diabetes-prone and diabetes-resistant BB rats: animal models of spontaneous and virally induced diabetes mellitus, lymphocytic thyroiditis, and collagen-induced arthritis. Guberski, D.L. Washington, Institute of Laboratory Animal Resources, National Research Council; 1993. ILAR news v. 35 (2): p. 29-37; 1993. Includes references. Language: English Descriptors: Rats; Disease models; Diabetes; Strain differences 97 NAL Call. No.: QP801.H7H65 Diabetic embryopathy and fuel-mediated organ teratogenesis: lessons from animal models. Freinkel, N. Stuttgart, W. Ger. : Georg Thieme; 1988 Aug. Hormone and metabolic research; Hormon- und Stoffwechselforschung; Hormones et metabolisme v. 20 (8): p. 463-475. ill; 1988 Aug. Includes references. Language: English Descriptors: Diabetes; Pregnancy; Maternal effects; Models; Abnormalities 98 NAL Call. No.: SF95.A1C6 Dietary effects in experimental carcinogenesis: animal models. Kritchevsky, D. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 174-185; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Literature review. Includes references. Language: English Descriptors: Animal models; Carcinogenesis; Dietary fat; Dietary protein; Carbohydrates; Restricted feeding; Trace elements; Vitamins; Literature reviews 99 NAL Call. No.: QP751.L5 Dietary fat and colon cancer: animal model studies. Reddy, B.S. Champaign, Ill. : American Oil Chemists' Society; 1992 Oct. Lipids v. 27 (10): p. 807-813; 1992 Oct. Paper presented at the "Symposium on Lipids in Cancer" held at the AOCS Annual Meeting, April 1990, Baltimore, Maryland. Includes references. Language: English Descriptors: Dietary fat; Fish oils; Fatty acids; Colon; Neoplasms; Carcinogenesis; Animal models; Reviews 100 NAL Call. No.: RA784.N8 Dietary fat and natural killer cell function. Byham, L.D. Baltimore, Md. : Williams & Wilkins; 1991 Jan. Nutrition today v. 26 (1): p. 31-36. charts; 1991 Jan. Literature review. Includes references. Language: English Descriptors: Natural killer cells; Dietary fat; Immunity; Neoplasms; Eicosanoids; Lymphocytes; Cell membranes; Lipoxygenase; Animal models; Clinical trials; Literature reviews Abstract: This article looks at the role of dietary fat in influencing the ability of natural killer cells to inhibit the proliferation of cancer cells. It includes: 1) an overview of the immune system; 2) a discussion of the lymphocytic membrane and; 3) a review of cyclo-oxygenase/lipoxygenase inhibition, and animal models and clinical trials on the role of eicosanoids in natural killer cell function. 101 NAL Call. No.: QP751.L5 Dietary fat and the development of pancreatic cancer. Roebuck, B.D. Champaign, Ill. : American Oil Chemists' Society; 1992 Oct. Lipids v. 27 (10): p. 804-806; 1992 Oct. Paper presented at the "Symposium on Lipids in Cancer" held at the AOCS Annual Meeting, April 1990, Baltimore, Maryland. Includes references. Language: English Descriptors: Dietary fat; Fatty acids; Fish oils; Calories; Exercise; Pancreas; Neoplasms; Carcinogenesis; Animal models; Rats; Reviews 102 NAL Call. No.: RA421.P684 Dietary fat, calories, and fiber in colon cancer. Reddy, B.S. Orlando, Fla. : Academic Press; 1993 Sep. Preventive medicine v. 22 (5): p. 738-749; 1993 Sep. Paper presented at the Fourth International Conference on Prevention of Human Cancer: Nutrition and Chemoprevention Controversies, June 3-6, 1992, Tucson, Arizona. Includes references. Language: English Descriptors: Carcinoma; Colon; Dietary fat; Fiber; Caloric intake; Carcinogenesis; Nutritional intervention; Literature reviews Abstract: The purpose of this presentation is (a) to provide an overview of the data thus far obtained in human epidemiological studies and laboratory animal models on the relationship between dietary fat, calories, and fiber and colon carcinogenesis and (b) to discuss whether the effect of dietary fat on colon carcinogenesis is due to the specific action of fat or to an associated caloric effect. Although the primary discussion of this presentation will be on laboratory animal model studies, reference will be made to human studies where appropriate. Future research will produce additional evidence for the etiologic role of types of dietary fat and fiber and total calories in cancer of the colon discussed in this presentation. 103 NAL Call. No.: RC620.A1J6 Dietary fat, calories, and the risk of breast cancer in postmenopausal women: a prospective population-based study. Barrett-Connor, E.; Friedlander, N.J. Wilmington, NC : American College of Nutrition; 1993 Aug. Journal of the American College of Nutrition v. 12 (4): p. 390-399; 1993 Aug. Includes references. Language: English Descriptors: Dietary fat; Energy intake; Mammary gland neoplasms; Nutrient intake; Menopause; Literature reviews; Risk; Women Abstract: We tested the hypothesis that a high-fat diet increases the risk of breast cancer in a population-based study of 590 women aged 40-79 years who were without known breast cancer when they provided a quantitative 24-hour diet recall. Fifteen postmenopausal women were diagnosed with incident breast cancer during the next 15 years (approximately 7600 person-years of follow-up). These women had significantly higher age-adjusted intake of afl fats (monounsaturated, polyunsaturated, and saturated), and oleic, linoleic, and linolenic acids, with a stepwise increase in risk across tertiles of intake. Fat intake was associated with total calories, protein, and carbohydrates, and women with incident breast cancer consumed more calories, protein, and carbohydrates than did other subjects. When each nutrient variable (calories, fats, protein, and carbohydrates) was adjusted for age, body mass index, age at menopause, parity, and alcohol consumption, the strongest risks for incident breast cancer were associated with total calories (relative risk per standard deviation = 2.72, 95% confidence interval = 1.51-4.89, p = 0.002) and total fats (relative risk per standard deviation = 2.01, 95% confidence interval = 1.19-3.41, p = 0.0 1). Fat composition of the diet, expressed either as percent of energy or as fat intake adjusted for calories by regression analysis, was not significantly associated with risk of breast cancer. These results support the hypothesis that total calorie consumption, as well as dietary fat consumption, is a risk factor for breast cancer in postmenopausal women, and parallel observations in animal models. 104 NAL Call. No.: QP751.L5 Dietary fat, fatty acids and prostate cancer. Rose, D.P.; Connolly, J.M. Champaign, Ill. : American Oil Chemists' Society; 1992 Oct. Lipids v. 27 (10): p. 798-803; 1992 Oct. Paper presented at the "Symposium on Lipids in Cancer" held at the AOCS Annual Meeting, April 1990, Baltimore, Maryland. Includes references. Language: English Descriptors: Dietary fat; Fatty acids; Prostate; Neoplasms; Obesity; Hormones; Growth factors; Risk; Animal models; Reviews 105 NAL Call. No.: QP141.A1N83 Dietary fibre in the prevention of colorectal cancer: lessons from studies in animal models. Young, G.P. South Perth, WA: The Society; 1990. Proceedings of the Nutrition Society of Australia v. 15: p. 112-119; 1990. Meeting held November 26-28, 1990, Adelaide, South Australia. Includes references. Language: English Descriptors: Fiber; Neoplasms; Colon 106 NAL Call. No.: QH301.F3 Dietary myristic, palmitic, and linoleic acids modulate cholesterolemia in gerbils. Pronczuk, A. \u Brandeis University, Waltham, MA; Khosla, P.; Hayes, K.C. Bethesda, Md. : The Federation of American Societies for Experimental Biology; 1994 Nov. The FASEB journal : official publication of the Federation of American Societies for Experimental Biology v. 8 (14): p. 1191-1200; 1994 Nov. Includes references. Language: English Descriptors: Meriones unguiculatus; Cholesterol; Blood plasma; Blood composition; Myristic acid; Linoleic acid; Fatty acids; Palmitic acid; Intake; Cholesterol metabolism; Hypercholesterolemia; Regression analysis; Animal models 107 NAL Call. No.: 447.8 AM3 Dietary obesity and weight cycling in rats: a model of stress- induced hypertension?. Contreras, R.J.; King, S.; Rives, L.; Williams, A.; Wattleton, T. Bethesda, Md. : American Physiological Society; 1991 Oct. American journal of physiology v. 261 (4,pt.2): p. R848-R857; 1991 Oct. Includes references. Language: English Descriptors: Obesity; Hypertension; Blood pressure; Heart rate; Stress; Diet; Body weight; Cycling; Angiotensin; Animal models; Rats Abstract: The present study was designed to reproduce the mild hypertension seen in dietary obese weight-cycled rats [P. Ernsberger and D. 0. Nelson. Am. J. Physiol. 254 (Regulatory Integrative Comp. Physiol 23): R47-R55, 1988] and determine whether this mild hypertension was associated with changes in sodium excretion and pressor responsiveness to angiotensin II (ANG II). Male Sprague-Dawley rats were fed pelleted chow (Pellet group) or chow plus sweetened condensed milk (Milk group) or were exposed to four cycles of a 4-day fast alternated with 2 wk of refeeding of pelleted chow and sweetened condensed milk (Cycled group). Blood pressure and heart rate were measured by tail cuff at the onset and last day of each fast and after 3 days of refeeding. During fasting, urine sodium excretion was measured. Mean arterial pressure and heart rate responses to intravenous administration of ANG II (40, 80, and 120 ng/kg), metoprolol (1 mg/kg), and methyl scopolamine (2 mg/kg) were obtained from the femoral artery in awake unrestrained rats. Weight cycling did not lead to mild hypertension or increased bradycardic response to sympathetic blockade with metoprolol. ANG II- elicited pressor responses were similar for Pellet, Milk, and Cycled groups. Sodium excretion did not change with fasting. Mild hypertension developed when obese weight-cycled rats were housed together in groups and not when housed individually. Our preliminary data are consistent with the notion that stress associated with group housing may be a factor in the mild hypertension of obese weight-cycled rats. 108 NAL Call. No.: RC692.D54 1990 Dietary proteins, cholesterol, metabolism and atherosclerosis. Sugano, Michihiro,_1933-; Beynen, Anton C., Basel ; New York : Karger,; 1990. 163 p. : ill. ; 25 cm. (Monographs on atherosclerosis ; vol. 16). Includes index. Includes bibliographical references. Language: English Descriptors: Atherosclerosis; Blood cholesterol; Hypercholesteremia; Food; Blood proteins Abstract: Analyzes the effects of dietary animal, vegetable and fish proteins on serum cholesterol levels in animal models and humans. Explores the possible mechanisms which have been advanced to date and reports the results of original research inquiries. 109 NAL Call. No.: SF95.A1C6 Dietary-induced obesity in experimental animals. Kanarek, R.B.; Orthen-Gambill, N. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 83-110; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Literature review. Includes references. Language: English Descriptors: Animal models; Rats; Obesity; Dietary fat; Dietary carbohydrate; Feed conversion efficiency; Feed intake; Adipose tissue; Fat metabolism; Nutritive ratio; Exercise; Carbohydrate metabolism disorders; Specific dynamic action; Literature reviews 110 NAL Call. No.: QP141.A1N88 Dimethylbenzanthracene-induced mammary tumorigenesis in ethanol-fed rats. Rogers, A.E.; Conner, B.H. Elmsford, N.Y. : Pergamon Press; 1990 Aug. Nutrition research v. 10 (8): p. 915-928; 1990 Aug. Includes references. Language: English Descriptors: Ethanol; Mammary gland neoplasms; Carcinogens; Rats Abstract: Epidemiological evidence indicates that ingestion of alcoholic beverages is a risk factor or is associated with a risk factor for breast cancer. A small increase in relative risk (1.1-1.2) compared to non-drinkers, has been reported for drinkers of small amounts of alcohol, approximately 3-4 drinks per week; a larger increase in relative risk (1.4-1.7) with a significant dose relationship occurs at intakes of 2-3 drinks per day. Two drinks per day would supply approximately 7-10% of a woman's caloric intake. This evidence, coupled with the general association of breast cancer risk with higher economic, nutritional and education status, supports the view that relevant animal models for study of the relationship between alcohol and breast cancer should employ moderate alcohol and good nutrient intake. Two carcinogenesis experiments were performed in ethanol-fed, female, Sprague- Dawley rats. In the first, groups of 50 rats were fed control diet ad libitum (CON) or were fed the diet with 20% of calories supplied as ethanol (ETOH) or were pair-fed control diet in amounts determined by the intake of ETOH rats (PF). They were given 7,12-dimethylbenzanthracene (DMBA), 20 mg/kg, by gavage at 55 days of age and monitored for tumor development. There was no detectable effect of ethanol on mammary tumor latency, incidence, number, weight or histology. In the second experiment, rats divided into the same groups were given 25% of calories as ethanol, with occasional increases to 35%, and the dose of DMBA was increased to 30 mg/kg. Again, there was no detectable effect of ethanol on mammary tumorigenesis. Thus, no effect of ethanol on mammary gland tumorigenesis by DMBA was observed in rats treated by 2 different protocols. 111 NAL Call. No.: 41.8 AM3A Dimethylnitrosamine-induced hepatotoxicosis in dogs as a model of progressive canine hepatic disease. Boothe, D.M.; Jenkins, W.L.; Green, R.A.; Corrier, D.E.; Cullen, J.M.; Boothe, H.W.; Weise, D. Schaumburg, Ill. : American Veterinary Medical Association; 1992 Mar. American journal of veterinary research v. 53 (3): p. 411-420; 1992 Mar. Includes references. Language: English Descriptors: Dogs; Hepatitis; Disease models; Animal models; N-nitrosodimethylamine Abstract: A model of toxin-induced progressive hepatitis is described in Beagles. The toxin, dimethylnitrosamine, was administered orally to 18 Beagles; 6 dogs comprised a control group. Clinical signs and laboratory test results were monitored as disease progressed and were used to determine the end point of disease. Following euthanasia, histologic lesions were scored and used to derive a total severity score for each dog. Severity scores were then used to allot the 18 dogs to 3 groups of hepatic disease, defined as mild, moderate, or severe. Changes in clinical laboratory test results, including tests of hepatic function, and clinical signs indicative of liver disease were described chronologically for all dogs. Group means of clinical laboratory test results and quantifiable clinical signs (eg, weight loss and ascitic fluid accumulation) were compared. This model offers several advantages, compared with other experimental models of canine hepatic disease. These include hepatospecificity, similarity to natural disease (eg, the development of multiple extrahepatic portosystemic shunts), and the ability to titrate the disease to a desired end point. The major disadvantages of this model were the toxic nature of the drug to human beings and the variation in individual animal response to the toxin, which precludes preassignment of animals into groups. 112 NAL Call. No.: 447.8 Am3 Direct plasma radioimmunoassay for rat amylin-(1-37): concentrations with acquired and genetic obesity. Pieber, T.R.; Roitelman, J.; Lee, Y.; Luskey, K.L.; Stein, D.T. Bethesda, Md. : American Physiological Society, 1898-; 1994 Jul. American journal of physiology v. 267 (1,pt.1): p. E156-E164; 1994 Jul. Includes references. Language: English Descriptors: Obesity; Polypeptides; Insulin; Measurement; Blood plasma; Radioimmunoassay; Aging; Pathogenesis; Animal models; Rats Abstract: Amylin (islet-associated polypeptide) is a 37-amino acid peptide that is cosecreted with insulin from the pancreatic beta-cell. Accurate measurement of its plasma levels is important for delineating the physiological range over which amylin acts. We describe a reproducible, highly specific, and sensitive radioimmunoassay for direct measurement of plasma amylin-(1-37). We measured changes in portal and systemic plasma amylin and insulin in three groups of anesthetized rats: lean young adult and old adult Wistar rats with acquired obesity, and Wistar fatty [WDF/TaFa (fa/fa)] rats, a model of genetic obesity and insulin resistance derived from the Wistar strain. Changes in response to fasting, feeding, and intravenous stimulation with glucose plus arginine were assessed. We find that the amylin-to- insulin ratio is constant in fasted or fed young and old rats because of proportionate increases in both entities with aging. In genetically obese Wistar rats, amylin and insulin levels are three- to tenfold higher than in lean young or obese old normal controls. Islet stimulation by feeding or intravenous glucose plus arginine resulted in a decreased amylin-to-insulin molar ratio in all groups. When normalized for the degree of islet stimulation, amylin-to-insulin ratios were significantly elevated in genetically obese vs. normal rats, both in the portal and systemic circulation. These results demonstrate that aging-related weight gain in normal rats is associated with moderate and proportional increases in amylin and insulin, whereas genetic obesity is characterized by elevated amylin and an increased amylin-to-insulin ratio. Implications for the pathogenesis of insulin resistance and obesity are discussed. 113 NAL Call. No.: QD1.A45 Discovery and development of novel prototype antibiotics for opportunistic infections related to acquired immunodeficiency syndrome. Clark, A.M.; Hufford, C.D. Washington, D.C. : American Chemical Society, 1974-; 1993. ACS symposium series (534): p. 228-241; 1993. In the series analytic: Human medicinal agents from plants / edited by A.D. Kinghorn and M.F. Balandrin. Includes references. Language: English Descriptors: Antibiotics; Plant extracts; Antifungal properties; Antimicrobial properties; Opportunistic infections; Screening; Acquired immune deficiency syndrome; Research Abstract: The major AIDS-related opportunistic fungal and bacterial infections are candidiasis. cryptococcosis and mycobacteriosis. The need for new, more effective and less toxic antibiotics for the treatment of these infections is obvious in light of the significant toxicities and failure rates of the currently available agents. In the past, the discovery of new antibiotics has relied primarily on the isolation of such agents from natural sources. The major advantage of this approach is the likelihood of identifying new prototype drugs with different chemical structures, and hence, possible new mechanisms and less likelihood of similar toxicities and cross-resistance. Although in the past microorganisms have been the primary source of new antibiotics, higher plants are now recognized as important sources of new antimicrobial agents. Recent efforts to discover new prototype antibiotics with potential utility specifically for the treatment of opportunistic disseminated mycoses and mycobacteriosis are discussed. Initial in vitro evaluation of higher plant extracts for antifungal and antimycobacterial activity is followed by fractionation and purification of active extracts using a bioassay-directed scheme. Pure compounds with significant in vitro activity are evaluated for in vivo efficacy in established animal models of disseminated mycosis and mycobacteriosis in order to determine their potential clinical utility. 114 NAL Call. No.: 49 J82 Divergent selection for immune responsiveness in chickens: estimation of realized heritability with an animal model. Pinard, M.H.; Arendonk, J.A.M. van; Nieuwland, M.G.B.; Zijpp, A.J. van der Champaign, Ill. : American Society of Animal Science; 1992 Oct. Journal of animal science v. 70 (10): p. 2986-2993; 1992 Oct. Includes references. Language: English Descriptors: Fowls; Line differences; Antibody formation; Animal models; Heritability; Selection responses; Genetic trend; Selection differential; Breeding value; Phenotypes Abstract: With the aim of improving general disease resistance, chickens were divergently selected for their antibody titers 5 d after immunization with sheep red blood cells for nine generations. Selected and control lines differed significantly for primary and secondary responses after three generations. Heritability of the antibody titer was estimated by REML fitting an animal model using a derivative-free algorithm. The heritability estimate using data on all lines simultaneously was .31. Realized heritability of the antibody titer in the selected lines was estimated by using either the phenotypic cumulative response as the deviation from the control line or the mean breeding values obtained with an animal model. Values from the two methods were consistent, giving a realized heritability of .21 and .25 in the high and low lines, respectively. The genetic trend was not linear and the response to selection tended to accelerate over generations. 115 NAL Call. No.: SF601.A47 The effect of a single oral dose of tri-o-cresyl phosphate on neurotoxic esterase and acetylcholinesterase activities in the central nervous system, erythrocytes and plasma. Barrett, D.S.; Oehme, F.W. Manhattan, Kan. : Kansas State University; 1994 Feb. Veterinary and human toxicology v. 36 (1): p. 1-4; 1994 Feb. Includes references. Language: English Descriptors: Organophosphorus compounds; Toxicity; Oral administration; Esterases; Acetylcholinesterase; Enzyme activity; Inhibition; Erythrocytes; Leukocytes; Blood plasma; Pigs; Animal models; Toxicology; Nervous system diseases 116 NAL Call. No.: QP501.C6 Effect of adenine metabolites on survival of Drosophila melanogaster of low xanthine dehydrogenase activity. Ho, Y.K.; Guthrie, M.J.; Clifford, A.J.; Ho, C.C. Oxford : Pergamon Press; 1992 Oct. Comparative biochemistry and physiology : B : Comparative biochemistry v. 103 (2): p. 413-417; 1992 Oct. Includes references. Language: English Descriptors: Drosophila melanogaster; Adenine; Metabolism; Metabolites; Toxicity; Survival; Xanthine dehydrogenase; Enzyme activity; Metabolic disorders; Animal models Abstract: Low xanthine dehydrogenase (LXD) mutant Drosophila melanogaster were fed 0.2% adenine for 7 generations, no adenine for the next 2 generations (relaxed) and 0.2% adenine again for the next 3 generations (rechallenged) to obtain adenine-resistant lines of Drosophila (LXD-adenine). Flies grown without adenine served as LXD-controls. Purines ranked as follows; adenine > adenosine > AMP > inosine > IMP in decreasing order of toxicity to LXD-adenine flies. Addition of ribose to 9N position, or phosphate or carboxy to 6C position of the purine ring alleviated the toxicity. More LXD-adenine offspring survived than did LXD-control offspring rechallenged with adenine. 117 NAL Call. No.: QP534.B56 Effect of age and sex on copper-induced toxicity in the macular mutant mouse--an animal model for Menkes' kinky-hair disease. Shiraishi, N.; Taguchi, T.; Kinebuchi, H. Totowa, N.J. : Humana Press; 1993 Nov. Biological trace element research v. 39 (2/3): p. 129-137; 1993 Nov. Includes references. Language: English Descriptors: Copper; Subcutaneous injection; Toxicity; Age; Sex; Disease models; Mice 118 NAL Call. No.: 381 J8282 Effect of dietary oils on lipid peroxidation and on antioxidant parameters of rat plasma and lipoprotein fractions. Scaccini, C.; Nardini, M.; D'Aquino, M.; Gentili, V.; Di Felice, M.; Tomassi, G. Bethesda, Md. : Lipid Research, Inc; 1992 May. Journal of lipid research v. 33 (5): p. 627-633; 1992 May. Includes references. Language: English Descriptors: Dietary fat; Soybean oil; Olive oil; Triolein; Unsaturated fatty acids; Antioxidants; Lipid peroxidation; Low density lipoprotein; Very low density lipoprotein; Blood lipids; Blood plasma; Rats Abstract: In order to investigate the influence of fatty acid pattern and antioxidants other than vitamin E on lipid peroxidation and antioxidant levels of plasma very low density and low density lipoproteins (VLDL + LDL), the effects of three diets (equalized for vitamin E) containing soybean oil, olive oil, or an oleate-rich mixture of triglycerides (triolein) were studied in rats. A significantly lower concentration of thiobarbituric acid-reactive substances (TBA- RS) in plasma and lipoproteins was found after the olive oil diet (soybean oil, 3.7 +/- 0.4 nmol/ml; triolein, 2.1 +/- 0.5 nmol/ml; olive oil, 1.5 +/- 0.3 nmol/ml, in plasma) (soybean oil, 0.99 +/- 0.16 nmol/ml; triolein, 0.96 +/- 0.13 nmol/ml; olive oil, 0.38 +/- 0.12 nmol/ml, in the VLDL + LDL fraction). Furthermore, the results from in vitro copper-induced lipid peroxidation, expressed in terms of conjugated dienes, lipid hydroperoxides, and TBA-RS content, showed that VLDL + LDL particles from olive oil-fed rats were remarkably resistant to oxidative modification. The results suggest that the fatty acid unsaturation of dietary oils is not the only determining factor of the antioxidant capacity of lipoproteins in this animal model. The maximal protection observed after the olive oil diet may be explained by the presence of other unidentified antioxidants in addition to vitamin E, derived from oil intake. Therefore, the optimal balance between the content of unsaturated fatty acids and natural antioxidants in dietary oils appears to be of major importance. 119 NAL Call. No.: RC628.N48 1987 The effect of different dietary carbohydrates on insulin and glucagon receptors in two models of genetic obesity: LA/N- corpulent rat and SHR/N-corpulent rat. Bhathena, S.J.; Kennedy, B.W.; Michaelis, O.E. IV; Jones, J.; Carswell, N.; Marsh, P.A.; Hansen, C.T.; Voyles, N.R.; Recant, L. Bethesda, Md. : National Institutes of Health; 1988. New models of genetically obese rats for studies in diabetes, heart disease, and complications of obesity : NIH workshop, June 18-19, 1987, summaries of workshop papers and current bibliography. p. 25-30; 1988. Includes references. Language: English Descriptors: Animal models; Obesity; Dietary carbohydrate; Glucagon; Insulin; Rats 120 NAL Call. No.: QP141.A1N88 The effect of ovarian status, form of vitamin D3 steroid and calcium supplementation on bone metabolism in the rat and the quail. Osborne, M.T.; Soares, J.H. Jr Elmsford, N.Y. : Pergamon Press; 1990 Aug. Nutrition research v. 10 (8): p. 887-901; 1990 Aug. Includes references. Language: English Descriptors: Cholecalciferol; Vitamin d; Metabolites; Osteoporosis; Bone density; Calcium; Mineral supplements; Ovariectomy; Rats; Quails Abstract: Degenerative bone conditions such as osteoporosis affect the elderly population by causing skeletal fractures. The incidence of osteoporosis is far greater in postmenopausal women and therefore, loss of ovarian function, leading to estrogen deficiency, plays an important role in the development of this disease. Abnormal vitamin D metabolism and insufficient dietary calcium may also contribute to the development of osteoporosis. Three experiments were conducted to investigate the effects of estrogen supplementation and dietary vitamin D3 steroids or calcium supplementation on skeletal metabolism. Eight week old ovariectomized (Ovx) or sham operated Sprague-Dawley rats or aged anovulatory Coturnix quail hens were used as animal models. Feeding a diet containing 1,25(OH)2D3 (5 microgram/kg) with 0.2% calcium was as effective in maintaining bone mineral concentrations as 20 microgram/kg vitamin D3 and 1.0% calcium. However, both bone calcium and zinc concentrations were decreased in Ovx rats and anovulatory quail fed 1,25(OH)2D3 and low calcium. Estrogen supplementation to Ovx rats and anovulatory quail fed 1,25(OH)2D3 and 0.2% Ca increased mineral concentrations, thus suggesting enhanced skeletal integrity. Therefore, these studies suggest improved skeletal calcification in control and estrogen supplemented female rats and quail fed 1,25(OH)2D3 and 0.2% calcium versus vitamin D3 with 1.0% calcium. 121 NAL Call. No.: 389.8 J824 Effect of phytate removal on zinc absorption from soy formula. Lonnerdal, B.; Bell, J.G.; Hendrickx, A.G.; Burns, R.A.; Keen, C.L. Baltimore, Md. : American Society for Clinical Nutrition; 1988 Nov. American journal of clinical nutrition v. 48 (5): p. 1301-1306. charts; 1988 Nov. Includes 28 references. Language: English Descriptors: Zinc; Infant formulas; Soy milk; Phytate; Intestinal absorption; Neonates; Rhesus monkeys; Rats Abstract: Low zinc bioavailability from soy formula may be the result of the formula's phytate content. We assessed the effect of phytate removal from soy formula on Zn absorption using infant rhesus monkeys and suckling rat pups as animal models. Zn absorption in monkeys, as determined by whole-body counting, was 65% from human milk, 54% from monkey milk, 60% from whey-predominant formula, 46% from casein-predominant formula, and only 27% from conventional soy formula (0.621 mmol phytate/L). In contrast, Zn absorption from dephytinized soy formula (0.067 mmol phytate/L) was 45%. In suckling rats, Zn absorption from conventional soy formula was only 16% vs 47% from dephytinized soy formula. Phytate concentration in a variety of experimental soy formulas was inversely correlated to Zn absorption. These results suggest that the low bioavailability of Zn from soy formula is a function of its phytate concentration and can be overcome by the removal of phytate. 122 NAL Call. No.: 381 B522 The effect of pravastatin on serum cholesterol levels in hypercholesterolemic diabetic rabbits. Arbeeny, C.M.; Bergquist, K.E. Amsterdam : Elsevier Science Publishers; 1991 Apr03. Biochimica et biophysica acta : International journal of biochemistry and biophysics v. 1096 (3): p. 238-244; 1991 Apr03. Includes references. Language: English Descriptors: Diabetes mellitus; Hypercholesterolemia; Drug therapy; Blood serum; Cholesterol; Rabbits Abstract: Diabetes mellitus is associated with hyperlipidemia and increased risk of atherosclerosis. A diabetic animal model has been developed to study the effect of treatment with pravastatin, a potent HMG CoA reductase inhibitor, on plasma lipoprotein levels. Hypercholesterolemia was induced in alloxan diabetic and control rabbits by feeding a diet containing 25% casein and 10% hydrogenated coconut oil for 8 weeks. Feeding the casein-coconut oil diet to the diabetic group resulted in a 5-fold increase in serum cholesterol levels, which was not statistically different from the nondiabetic group fed this diet. However, in the diabetic group, there was more cholesterol in the VLDL fraction and less in LDL as compared to the nondiabetic group. Serum triacylglycerol levels in the diabetic rabbits were variable and ranged from 58-943 mg/dl. The diabetic and nondiabetic animals were then treated with pravastatin at a dose of 10 mg/kg per day for 21 days. In the nondiabetic group, pravastatin treatment significantly lowered serum and LDL cholesterol concentrations by 28.5% (52.3 mg/dl, P < 0.05) and 36.2% (40.7 mg/dl, P < 0.05) respectively, relative to the placebo group. Serum and VLDL triacylglycerol levels in the nondiabetic group were also significantly decreased following pravastatin treatment. In the diabetic group, serum and LDL cholesterol levels were decreased by 37.0% (69.1 mg/dl, P < 0.05) and 52.7% (32.1 mg/dl, P < 0.01), respectively, relative to the diabetics given the placebo. Pravastatin treatment did not adversely affect serum glucose levels. Thus, pravastatin treatment was effective in controlling the hypercholesterolemia present in these diabetic animals. 123 NAL Call. No.: 41.8 J82 The effect of recent vaccination on the dose-response to experimental Dermatophilus congolensis infection in rabbits. How, S.J.; Lloyd, D.H. London : Academic Press; 1990 Feb. Journal of comparative pathology v. 102 (2): p. 157-163; 1990 Feb. Includes references. Language: English Descriptors: Rabbits; Dermatophilus congolensis; Vaccination; Live vaccines; Dosage effects; Elisa; Cross immunity; Cross immunization; Animal models 124 NAL Call. No.: RC262.C5N8 Effect of the amount of dietary fat on the development of mammary tumors in BALB/c-MTV mice. Zevenbergen, J.L.; Verschuren, P.M.; Zaalberg, J.; Stratum, P. van; Vles, R.O. Hillsdale, N.J. : Lawrence Erlbaum Associates, Inc; 1992. Nutrition and cancer v. 17 (1): p. 9-18; 1992. Includes references. Language: English Descriptors: Dietary fat; Mammary gland neoplasms; Incidence; Mice Abstract: The relationship between dietary fat consumption and the incidence of breast cancer, if any, needs to be quantified so that dietary guidelines can be issued for the prevention of breast cancer. Frequently, only two widely different dietary fat levels, often differing in essential fatty acid content, have been compared in animal models. Moreover, the latent period in common animal models for breast cancer is very short and does not reflect the relatively long latent periods in human breast cancer. We describe a study with BALB/c-MTV mice, a strain with a high average tumor incidence and a latent period of over 60 weeks on average. The mice were fed diets with fat levels ranging from 10% to 40% of energy, in which fat was isocalorically substituted for carbohydrates. The level of linoleic acid in these diets was kept constant al 6.5% of energy. Both the mean tumor incidence and latent periods of the groups fed diets with 10-16% of energy as fat were not significantly different from each other. There were also no differences between these parameters in the groups fed 22-40% of energy as fat. However, the mean incidence and latent period of the groups fed 22% or more of energy as fat was significantly higher than that of the groups fed less fat. We conclude that above about 22 % of energy, fat does not influence the incidence and latent period of mammary tumors in BALB/c-MTV mice. 125 NAL Call. No.: 41.8 AM3A Effectiveness of arprinocid in the reduction of cryptosporidial activity in immunosuppressed rats. Rehg, J.E.; Hancock, M.L. Schaumburg, Ill. : American Veterinary Medical Association; 1990 Oct. American journal of veterinary research v. 51 (10): p. 1668-1670; 1990 Oct. Includes references. Language: English Descriptors: Cryptosporidium; Rats; Immunosuppression; Arprinocid; Drug effects; Disease prevention Abstract: Immunosuppressed rats inoculated with Cryptosporidium oocysts isolated from calves' feces were treated with arprinocid, 50 mg/kg of body weight/d. As determined from differences in the mean number of cryptosporidial developmental stages per villus in treated vs control rats, arprinocid had a substantial effect on cryptosporidial activity, which was parasitistatic instead of parasiticidal. Drug-ranging experiments indicated that arprinocid was effective at 50 and 25 mg/kg/d, but not at 12.5 mg/kg/d. These results suggest that further testing of arprinocid in different animal models, or in phase-I clinical trials, is warranted. 126 NAL Call. No.: 410.9 P94 Effects of dieatary vitamin E on clinical course and plasma glutamic oxaloacetic transaminase and glutamic pyruvic transaminase activities in hereditary hepatitis of LEC rats. Yamazaki, K.; Ohyama, H.; Kurata, K.; Wakabayashi, T. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Feb. Laboratory animal science v. 43 (1): p. 61-67; 1993 Feb. Includes references. Language: English Descriptors: Rats; Hepatitis; Vitamin e; Animal models Abstract: Long-Evans Cinnamon (LEC) rats are autosomal recessive mutants that develop hepatitis and hepatocellular carcinoma. Because copper accumulates in the livers of these rats, and some of their clinical and pathological features are similar to those of patients with Wilson's disease, LEC rats are proposed as an animal model of Wilson's disease. It has been thought that unbound copper generates free radicals, which act as hemolytic and hepatocytotoxic agents. To examine the effects of vitamin E as an antioxidant on hereditary hepatitis in LEC rats, we fed 3-week-old rats for 25 weeks either vitamin E-deficient, control, or vitamin E-supplemented diets which contained < 0.1 mg of total tocopherols, 2 mg of d,l-alpha-tocopheryl acetate (2 I.U.), and 58.5 mg of d,l- alpha-tocopheryl nicotinate (50 I.U.), respectively, per 100 mg of feed. In males, body weight loss was first observed in the vitamin E-deficient group, and mean ages at which jaundice occurred were in the order: deficient younger than control younger than supplemented groups. The ages when plasma glutamic oxaloacetic transaminase and glutamic pyruvic transaminase activities began to increase sharply and peaked followed the same order. Thus, it is likely that free radicals are involved in jaundice and hepatitis in LEC male rats, and they are a model for studying the relationship of copper, free radicals, and hepatitis. Conversely, in females, no apparent differences in clinical and biochemical changes were observed among the three groups. Causes for the discrepancy between the sexes remain to be clarified. 127 NAL Call. No.: QP141.A1N88 Effects of dietary fish oil on survival and renal fatty acid composition in murine polycystic kidney disease. Aukema, H.M.; Yamaguchi, T.; Takahashi, H.; Philbrick, D.J.; Holub, B.J. Tarrytown, N.Y. : Pergamon Press; 1992 Nov. Nutrition research v. 12 (11): p. 1383-1392; 1992 Nov. Includes references. Language: English Descriptors: Diet; Fish oils; Kidney diseases; Kidneys; Fatty acids; Composition; Mice Abstract: It has been demonstrated that replacing dietary n-6 with n-3 polyunsaturated fatty acids is beneficial in some animal models of renal disease, but not in others. We fed semi-purified diets containing either sunflowerseed oil (containing linoleic acid, 18:2n-6) or fish oil (containing eicosapentaenoic acid, 20:5n-3, plus docosahexaenoic acid, 22:6n-3) to a mouse model of polycystic kidney disease (DBA/2FG-pcy). Renal phospholipid and triglyceride fatty acid compositions were markedly altered by dietary treatment: 20:5n-3 and 22:6n-3 levels were elevated in the kidneys from mice fed fish oil at the expense of 18:2n-6 and arachidonic acid, 20:4n-6. Despite these lipid alterations, however, survival and proteinuria were not improved by long term fish oil consumption in mice with polycystic kidney disease. 128 NAL Call. No.: RC628.A1O2 Effects of exercise and stress on body fat distribution in male cynomolgous monkeys. Jayo, J.M.; Shively, C.A.; Kaplan, J.R.; Manuck, S.B. Avenel, NJ : The Macmillan Press Ltd; 1993 Oct. International journal of obesity and related metabolic disorders : journal of the International Association for the Study of Obesity v. 17 (10): p. 597-604; 1993 Oct. Includes references. Language: English Descriptors: Body fat; Distribution; Exercise; Mental stress; Nutrient intake; Computed tomography; Males; Monkeys Abstract: The effects of exercise and stress on regional and whole body adiposity were examined in an established animal model of diet-induced coronary artery atherosclerosis, the cynomolgus monkey (Macaca fascicularis). A total of 79 adult male monkeys were assigned to four experimental groups after baseline stabilization and training: (i) exercise, stress, (n = 20); (ii) exercise, no stress (n = 20); (iii) sedentary, stress (n = 20); and (iv) sedentary, no stress (n = 19). The monkeys consumed an ad libitum diet containing 188 mg cholesterol per day with 43% of calories as saturated fat. Anthropometric measurements of regional and whole body adiposity were collected throughout the study. A subset (n = 40) of animals representing all four groups underwent computerized tomography (CT) scans at the end of the study to determine amounts of total abdominal, intra-abdominal and subcutaneous abdominal adipose tissue. Results indicate that, in general, stress interacted with exercise to affect anthropometric measurements of regional adiposity. In contrast, stress had independent and significant effects on the amount and distribution of abdominal fat as measured using CT. Stressed monkeys in both the exercise and sedentary groups had more intra-abdominal fat (and thus greater intra-abdominal- :subcutaneous abdominal fat ratios) than their non-stressed counterparts. There were no significant interactions between exercise and stress or exercise effects on abdominal fat distribution as measured by CT. These results support the belief that an arousal syndrome caused by chronic stress, and resulting in increased activity along the hypothalamo-adrenal axis, may play a role in the preferential deposition of fat in the abdomen. Finally, anthropometric measurements did not predict the proportion of intra-abdominal versus subcutaneous fat in abdominal depots, suggesting that anthropometric measurements and CT assess different characteristics of fat distribution. 129 NAL Call. No.: RC620.A1J6 Effects of gestation, lactation, and maternal calcium intake on mechanical strength of equine bone. Glade, M.J. Wilmington, NC : American College of Nutrition; 1993 Aug. Journal of the American College of Nutrition v. 12 (4): p. 372-377; 1993 Aug. Includes references. Language: English Descriptors: Calcium; Nutrient intake; Lactation; Pregnancy; Bone strength; Postpartum period; Maternal nutrition; Horses Abstract: Skeletal homeostasis during late gestation, lactation, and the post-lactational recovery period is poorly understood. In an experiment using an animal model (the horse), metacarpal breaking strengths (MBS) estimated via transmission ultrasonics were examined during the last 12 weeks of gestation and for 40 weeks after parturition. MBS increased during the last 6-10 weeks of gestation in mares fed amounts of calcium (Ca) recommended by the National Research Council; maximum MBS coincided with the week of parturition. In contrast, MBS in mares fed 20% less Ca remained relatively constant during the last 12 weeks of gestation. In contrast to increases during late gestation, MBS decreased steadily in all mares during the first 12 weeks of lactation. MBS increased after approximately 12 weeks of lactation, but more slowly than they had declined. MBS of the bones of mares fed recommended amounts of Ca were fully restored at 24 weeks post-parturition, but those of Ca-deficient mares had not fully recovered even 20 weeks after milk production had ceased (40 weeks after parturition). Mid-cannon mediolateral diameters of foals born to mares fed Ca-deficient diets were thinner and mechanically weaker at birth (both p < 0.01). These differences in limb bone size and strength persisted during the first 40 weeks of life. 130 NAL Call. No.: 448.8 M56 Effects of high fat-feeding to rats on the interrelationship of body weight, plasma insulin, and fatty acyl-coenzyme A esters in liver and skeletal muscle. Chen, M.T.; Kaufman, L.N.; Spennetta, T.; Shrago, E. Philadelphia, Pa. : W.B. Saunders Co; 1992 May. Metabolism: clinical and experimental v. 41 (5): p. 564-569; 1992 May. Includes references. Language: English Descriptors: Dietary fat; Saturated fats; Dietary carbohydrate; Body weight; Blood plasma; Insulin; Glucose; Energy intake; Acetyl coenzyme a; Liver; Skeletal muscle; Hyperinsulinemia; Correlation; Lipid metabolism; Carbohydrate metabolism; Animal models; Rats 131 NAL Call. No.: 500 N484 Effects of marine fish oil on blood pressure and vascular reactivity in the hereditary hypertriglyceridemic rat. Edelsteinova, S.; Kyselovic, J.; Klimes, I.; Sebokova, E.; Kovacsova, B.; Kristek, F.; Mitkova, A.; Vrana, A.; Svec, P. New York : New York Academy of Sciences, 1877-; 1993. Annals of the New York Academy of Sciences v. 683: p. 353-356; 1993. In the series analytic: Dietary lipids and insulin action / edited by I. Klimes, B.V. Howard, L.H. Storlien, and E. Sebokova. Proceeding of the Second International Smolenice Insulin Symposium, September 12-16, 1992, Smolenice Castle, Slovak Republic. Includes references. Language: English Descriptors: Animal models; Blood pressure; Fish oils; Food supplements; Human nutrition research; Hereditary diseases; Hypertriglyceridemia; Rats 132 NAL Call. No.: RC628.A1O2 Effects of maternal obesity on fasting metabolism in newborn rats. Heng, J.; Kliegman, R.M. Basingstoke, Hampshire : The Macmillan Press Ltd; 1990 Jun. International journal of obesity v. 14 (6): p. 505-513; 1990 Jun. Includes references. Language: English Descriptors: Obesity; Maternal nutrition; Fasting; Metabolism; Hypoglycemia; Weight gain; Pregnancy; Eating patterns; Neonates; Rats Abstract: Maternal obesity is a risk factor for subsequent fasting hypoglycemia in human infants after birth. To investigate further this problem, we employed an animal model of obesity to study neonatal extrauterine metabolic adaptations in pups of obese and lean rats. Female Sprague- Dawley rats were fed a 'cafeteria diet' to induce obesity prior to and during pregnancy. Prior to mating, the cafeteria fed rats were significantly heavier (449 v. 345 g, P < 0.001) than the controls. Furthermore, weight gain during pregnancy and weight at term were also significantly greater in the obese rats even though they consumed less food during pregnancy. Pup weights and the number of pups per litter were similar between the two groups. Pups born to obese mothers demonstrated hypoglycemia after being fasted for 150 and 180 min when compared with control pups. Hepatic glycogen stores were increased in the fetus of pups born to obese mothers. Glycogen content in pups born to obese mothers declined minimally after birth and remained greater than hepatic glycogen values in control pups throughout the study. In addition to increased fetal storage of glycogen, fetal hepatic triglyceride content was augmented in pups of obese rats. These triglyceride stores declined and were mobilized during fasting after birth. In contrast, hepatic triglyceride content increased after birth among control rats. These results suggest that maternal obesity results in augmented fetal hepatic tissue stores of both glycogen and triglycerides. Hypoglycemia among pups of excessively obese mothers may be due to attenuated mobilization of hepatic glycogen. Alternate fuel utilization as evident by the mobilization (rather than storage) of hepatic triglycerides may contribute to energy metabolism during periods of hypoglycemia. 133 NAL Call. No.: RC620.A1N8 The effects of replacing coconut oil with corn oil on human serum lipid profiles and platelet derived factors active in atherogenesis. Mendis, S.; Wissler, R.W.; Bridenstine, R.T.; Podbielski, F.J. Stoneham, Mass. : Butterworth; 1989 Oct. Nutrition reports international v. 40 (4): p. 773-782. charts; 1989 Oct. Includes 33 references. Language: English Descriptors: Sri lanka; Maize oil; Coconut oil; Diet; Blood lipids; Cholesterol; Triglycerides; High density lipoprotein; Low density lipoprotein; Young adults; Men Abstract: Young, healthy individuals living in Sri Lanka often consume a diet containing coconut oil as their main source of fat. Blood lipid values and selected platelet related factors have been measured in a group of 16 free living young adults, ages 16 to 21, before and 8 weeks after they had been shifted from their usual diet to a similar one in which the coconut oil was replaced by whole milk powder and corn oil. The results indicate that their blood cholesterol, cholesteryl ester, and several other related circulating blood lipid values, as well as the platelet factor 4 values, were elevated prior to the diet change. Many of these factors, associated as risk factors for atherogenesis, were substantially reduced at the end of the diet change. The only plasma components which were altered substantially were the triglycerides and the HDL cholesterol. These results suggest that the special atherogenic effects of coconut oil that have been demonstrated in so many animal models may be similarly active in humans. 134 NAL Call. No.: 410.9 P94 Effects of sex hormones on fulminant hepatitis in LEC rats: a model of Wilson's disease. Kasai, N.; Miyoshi, I.; Osanai, T.; Yamashita, T.; Kamimura, E.; Yoshida, M.C. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Aug. Laboratory animal science v. 42 (4): p. 363-368; 1992 Aug. Includes references. Language: English Descriptors: Rats; Disease models; Sex hormones; Hepatitis Abstract: LEC rats, which have hereditary hepatitis and have recently been proposed as an animal model for Wilson's disease, were examined to determine the effects of sex hormones on fulminant hepatitis. After the rats had undergone ovariectomies or orchidectomies (castration) and were compared with intact rats, the age at the onset of fulminant hepatitis was not substantially altered but the survival rates decreased from 50% to 12.5% for females and 75% to 14.3% for males, indicating that sex hormones did not influence the occurrence of fulminant hepatitis but influenced mortality due to fulminant hepatitis. When testosterone was administered to the ovariectomized or orchidectomized rats, the survival rate increased to over 90% in both sexes. In contrast, estradiol did not affect the survival rate of either sex but affected the onset of fulminant hepatitis. That is, with the administration of estradiol, the age at which serum GPT activity reached its maximum was delayed 4 weeks in ovariectomized rats and 6 weeks in orchidectomized rats as compared with intact rats. A similar but somewhat weaker tendency appeared in rats given progesterone. The results of our study indicate that sex hormones have no effect on the rate of occurrence of hepatitis but affect the progression of hepatitis. In particular, testosterone increased the survival rate of rats with fulminant hepatitis, and exogenous estradiol delayed the onset of hepatitis for several weeks. 135 NAL Call. No.: 44.8 J822 Efficacy of tumor necrosis factor-alpha and antibiotics in therapy of experimental murine staphylococcal mastitis. Sanchez, M.S.; Ford, C.W.; Yancey, R.J. Jr Champaign, Ill. : American Dairy Science Association; 1994 May. Journal of dairy science v. 77 (5): p. 1259-1266; 1994 May. Includes references. Language: English Descriptors: Tumor necrosis factor; Staphylococcus aureus; Mastitis; Animal models; Mice; Neutrophils; Lymphocyte transformation; Experimental infections; Bacterial count; Drug combinations; Ciprofloxacin; Cloxacillin; Antibiotics; Drug effects; Lactation; Dry period Abstract: The mouse model was used to determine the efficacy of the cytokine, tumor necrosis factor-alpha and antibiotic in treatment of experimentally induced staphylococcal mastitis. Recombinant human tumor necrosis factor-alpha alone administered to the mammary glands of lactating mice recruited significantly more polymorphonuclear neutrophils into the gland by 4 h posttreatment than did the untreated control. One hundred times less recombinant mouse tumor necrosis factor- alpha than human tumor necrosis factor-alpha was required to enhance the killing of Staphylococcus aureus within the gland. Human tumor necrosis factor-alpha effectively enhanced the killing of the bacteria when it was administered 4 to 0 h prior to infection, but not 4 h after infection. When mice were first pretreated with tumor necrosis factor-alpha, infected, and then treated with antibiotics (ciprofloxacin and pirlimycin, but not cloxacillin), the combination of antibiotic and cytokine significantly reduced the number of bacteria within the gland compared with that for mice treated with antibiotic alone, cytokine alone, or placebo. Recombinant tumor necrosis factor-alpha may be an effective adjunct to antimicrobial therapy in treatment of staphylococcal mastitis in the bovine. 136 NAL Call. No.: 41.8 AM3A Electrocadiographic and echocardiographic features of trypanosomiasis in dogs inoculated with North American Trypanosoma cruzi isolates. Barr, S.C.; Holmes, R.A.; Klei, T.R. Schaumburg, Ill. : American Veterinary Medical Association; 1992 Apr. American journal of veterinary research v. 53 (4): p. 521-527; 1992 Apr. Includes references. Language: English Descriptors: Louisiana; Dogs; Trypanosoma cruzi; Trypanosomiasis; Cardiomyopathy; Disease models; Electrocardiograms; Recordings; Disease course; Animal models Abstract: Purebred Beagles were inoculated with Trypanosoma cruzi isolates from a North American opossum or armadillo (Tc- W), and dog (Tc-D). Although Tc-D established infection in dogs, the dogs did not develop cardiac abnormalities. Dogs inoculated with Tc-W developed acute myocarditis associated with increases in P-R interval, atrioventricular block, depression of R wave amplitude and shifts in mean electrical axis. Echocardiograms were normal during this stage. Three Tc- W-inoculated dogs died during the acute stage. Following the acute stage, 5 of 8 Tc-W-inoculated dogs entered an indeterminate stage in which ECG changes were minor and echocardiograms were normal. Progression to the chronic stage in 5 of the 8 Tc-W-inoculated dogs was indicated by development of ventricular-based arrhythmias, mainly ventricular premature contractions, between postinoculation days 60 and 170. In some dogs, ventricular premature contractions were multifocal. Electrocardiographic abnormalities progressively degenerated to various forms of ventricular tachycardia. Worsening ECG coincided with loss of left ventricular function as measured by echocardiography. Mean percent ejection fraction and percentage of fractional shortening decreased to 63% and 52% of control values, respectively. The left ventricular free wall (LVFW) thickness decreased and % septal: % LVFW thickening ratio increased, indicating a relative preservation of septal wall motion and LVFW hypokinesis. 137 NAL Call. No.: 442.8 Ex7 Energy metabolism, replicative ability, intracellular calcium concentration, and ionic channels of horse articular chondrocytes. Vittur, F.; Grandolfo, M.; Fragonas, E.; Godeas, C.; Paoletti, S.; Pollesello, P.; Kvam, B.J.; Ruzzier, F.; Starc, T.; Mozrzymas, J.W. Orlando, Fla. : Academic Press; 1994 Jan. Experimental cell research v. 210 (1): p. 130-136; 1994 Jan. Includes references. Language: English Descriptors: Horses; Cartilage; Chondrocytes; Energy metabolism; Glycolysis; Replication; Calcium; Potassium; Phosphorus; Ion transport; Disease models; Arthritis Abstract: Some aspects of the physiology of chondrocytes from horse articular cartilage were studied, since this animal model can be helpful in understanding arthritic processes. The replicative ability of articular chondrocytes, measured by the incorporation of [3H]thymidine, and their capacity of proteoglycan production, evaluated from the incorporation of [35S]sulfate, are very low. In addition, these cells do not differentiate in vitro as shown by the constant specific activity of alkaline phosphatase measured at different times in culture. Two types of potassium channels were identified by patch clamp experiments in the cell-attached configuration, one characterized by a conductance of 40 pS and the other of 100 pS. No active K+ channels were found at V(pip) = 0. It was shown by Fura-2 experiments that the low replicative ability is paralleled by a modest variation of the intracellular calcium concentration after a mitogenic stimulus. 31P NMR experiments, both on slices of whole articular cartilage and on isolated cells, demonstrate that chondrocytes derive their energy mainly from the glycolytic pathway. 138 NAL Call. No.: 41.2 H198 1988 [no.108] Entwicklung eines Modelles zur Untersuchung psychosozialer und genetischer Einflusse auf den Verlauf einer chronisch respiratorischen Erkrankung (Murine Respiratorische Mykoplasmose) bei der Ratte [Development of an animal model to estimate social and genetic influences on the course of chronic respiratory disease (Murine Respiratory Mycoplasmosis)]. Iglauer, Franz Hannover : [s.n.],; 1988. 116 p. : ill. ; 21 cm. (Inaugural-Dissertation / Tierarztliche Hochschule Hannover ; 1988, [no. 108]). English summary. Includes bibliographical references. Language: German 139 NAL Call. No.: QR360.J6 Equine H7N7 influenza A viruses are highly pathogenic in mice without adaptation: potential use as an animal model. Kawaoka, Y. Washington, D.C. : American Society for Microbiology; 1991 Jul. Journal of virology v. 65 (7): p. 3891-3894; 1991 Jul. Includes references. Language: English Descriptors: Equine influenzavirus; Pathogenicity; Virulence; Fatal infections; Experimental infections; Nervous system diseases; Mice; Animal models Abstract: Equine H7N7 influenza A viruses, representing a broad range of isolates, were lethal in mice without adaptation. After repeated passages, A/Equine/London/1416/73 acquired neurotropism upon intranasal infection. Thus, mice infected with equine influenza A viruses provide a model system for the study of highly virulent mammalian influenza viruses. 140 NAL Call. No.: SF951.J65 Equine infectious anemia as an AIDS animal model. Tashijan, R.J.; Crusberg, T.C. Lake Elsinore, Calif. : William E. Jones, DVM; 1989 Mar. Journal of equine veterinary science v. 9 (2): p. 105-110; 1989 Mar. Literature review. Includes references. Language: English Descriptors: Horses; Equine infectious anemia; Equine infectious anemia virus; Disease models 141 NAL Call. No.: 389.1 W892 Essentiality of omega 3 fatty acids: evidence from the primate model and implications for human nutrition. Connor, W.E.; Neuringer, M.; Reisbick, S. Basel : S. Karger; 1991. World review of nutrition and dietetics v. 66: p. 118-132; 1991. In the series analytic: Health effects of omega-3 polyunsaturated fatty acids in seafoods / edited by A. Simopoulos, R. Kifer, R. Martin and S. Barlow. Includes references. Language: English Descriptors: Docosenoic acids; Fish oils; Essential fatty acids; Animal models; Macaca mulatta; Fat deficiencies; Experimental diets; Safflower oil; Blood plasma; Tissues; Fatty acids; Phospholipids; Vision disorders; Polydipsia Abstract: This study shows that dietary omega-3 fatty acid deficiency leads to severe and progressive depletion of omega-3 fatty acids from the plasma and from all tissues analyzed including red blood cells, liver, skin, fat, cerebral cortex and retina in primates. It supports the conclusion that there should be adequate amounts of both omega-3 and omega-6 fatty acids in the diet throughout life and that their ratio is of great importance. 142 NAL Call. No.: 410.9 P94 Evaluation of a nude mouse tumor model using beta- galactosidase-expressing melanoma cells. Dooley, T.P.; Stamp-Cole, M.; Ouding, R.J. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Feb. Laboratory animal science v. 43 (1): p. 48-57; 1993 Feb. Includes references. Language: English Descriptors: Mice; Animal models; Melanoma Abstract: We developed and evaluated an in vivo athymic nude mouse model for tumor growth, angiogenesis, metastasis, and antineoplastic drug development. Melanoma cell lines expressing beta-galactosidase encoded by the Escherichia coli lac Z gene have been created by infecting an immortal murine melanocyte cell line with a recombinant retrovirus expressing the v-Ha-ras oncogene and lac Z to generate the MRB (melanoma, ras, beta-galactosidase) cell lines. The amelanotic, phorbol ester-independent, transformed melanoma cell lines developed tumors rapidly when injected subcutaneously into nude mice, as well as experimental lung metastases when injected i.v. into the tail vein. beta-galactosidase-expressing subcutaneous tumors and lung metastases stained blue with X-gal. The melanomas produced in nude mice have been characterized by using various histochemical and immunohistochemical staining methods to detect melanoma- and endothelial-cell-specific markers to determine the extent of neovascularization in MRB nude mouse tumors. Optimal staining of endothelial cells involved in tumor angiogenesis was observed by using ADPase activity and antiangiotensin-converting enzyme antibody staining. Attempts at indirect quantification of metastatic tumor cell number within the lung by either beta-galactosidase enzymatic activity or ELISA immunoreactivity were unsuccessful. However, the MRB cell lines should be useful in screening for and studying the mechanisms of action of antineoplastic, antimetastatic, and angiostatic drugs in vivo in athymic nude mice. 143 NAL Call. No.: QL55.A1L3 Evaluation of inbred germ-free Fischer 344 albino rats as an experimental model for oral candidiasis. Van Wyk, C.W.; Basson, N.J.; Gibson, B.M. London : Royal Society of Medicine Services; 1989 Jul. Laboratory animals v. 23 (3): p. 248-255. ill; 1989 Jul. Includes references. Language: English Descriptors: Rats; Candidosis; Candida albicans; Tongue lesions; Tongue; Opportunistic infections; Germfree state; Inbred strains; Induced resistance; Animal models; Disease models Abstract: Inbred germ-free Fischer 344 albino rats were evaluated as models for experimental candidiasis in order to investigate bacterial interaction with Candida albicans. Female rats were exposed to C. albicans in their drinking water and killed at intervals from 2 to 22 days after initial contact with the contaminant. C. albicans was cultured from their mouths from day 2 but from day 12 the number of colonies decreased. From day 2 to 9 all rats showed oral histological signs of candidal infestation, but after 9 days the number declined to 3 out of 9 at 22 days. The dorsal surface of the tongue was the best histological indicator of candidal infestation. All the rats had tongue lesions from day 4 to 9, and from day 6 there was also a concomitant localized loss of filiform papillae. The number of rats with all forms of tongue involvement also decreased after 9 days with only 3 out of 9 affected at 22 days. It is concluded that Fischer 344 inbred germ-free rats can be used on a limited scale as a model for candidiasis and bacterial interaction with C. albicans, the dorsal surface of the tongue would be the best site for studying candidal experimental lesions and it is probable that better results can be achieved with complete standardization of contamination and preparation procedures. 144 NAL Call. No.: TD172.A7 Evaluation of the polychlorobiphenyl Aroclor 1254 in an animal model of atherosclerosis. Carter, J.W.; Koo, S.I. New York, N.Y. : Springer-Verlag; 1988 May. Archives of environmental contamination and toxicology v. 17 (3): p. 307-312; 1988 May. Includes references. Language: English Descriptors: Experimental atherosclerosis; Animal experiments; Polychlorinated biphenyls; Arochlor; Diets; Cholesterol; Pigeons 145 NAL Call. No.: RB127.P34 Experimental approach to reflex sympathetic dystrophy and related syndromes. Janig, W. Amsterdam : Elsevier Science Publishers; 1991 Sep. Pain : the journal of the International Association for the Study of Pain v. 46 (3): p. 241-245; 1991 Sep. Includes references. Language: English Descriptors: Rats; Animal models; Disease models; Nervous system diseases 146 NAL Call. No.: 41.8 R312 Experimental infectaion of the mouse mammary gland with Campylobacter coli. Diker, K.S.; Haziroglu, R.; Diker, F.S. London : British Veterinary Association; 1992 Jan. Research in veterinary science v. 52 (1): p. 123-125; 1992 Jan. Includes references. Language: English Descriptors: Campylobacter; Bovine mastitis; Disease models; Animal models; Mice; Mammary glands; Experimental infection; Strain differences Abstract: Campylobacter cob strains of bovine and avian origin were inoculated into the mammary gland of mice. A bovine strain isolated from a case of mastitis produced gross and histological changes in most of the glands; one bovine and one avian faecal isolate did not. Histologically, lesions were characterised by neutrophil infiltration in the alveolar spaces and necrosis and oedema in the interalveolar tissue. On bacteriological examination, the bovine mastitis strain could be isolated from most of the glands, but neither of the faecal strains. The mouse, therefore, appears to provide a convenient model for studying campylobacter mastitis. 147 NAL Call. No.: QR1.I57 Experimental infection of severe combined immunodeficient beige mice with Mycobacterium paratuberculosis of bovine origin. Mutwiri, G.K.; Butler, D.G.; Rosendal, S.; Yager, J. Washington, D.C. : American Society for Microbiology; 1992 Oct. Infection and immunity v. 60 (10): p. 4074-4079; 1992 Oct. Includes references. Language: English Descriptors: Cattle; Mice; Disease models; Mycobacterium paratuberculosis; Enteritis; Experimental infection; Cachexia; Pathogenesis; Immunological deficiency; Histology Abstract: Severe combined immunodeficient beige mice were inoculated orally and intraperitoneally with a bovine strain of Mycobacterium paratuberculosis to explore their potential as laboratory animal models in the study of paratuberculosis (Johne's disease). Control animals were similarly inoculated with heat-killed M. paratuberculosis. In the mice inoculated intraperitoneally, focal lesions and acid-fast bacilli were first detected in the livers (4 weeks postinfection) and later in the spleens and intestines of the test but not the control animals. No bacteria were seen in the hearts, kidneys, or lungs. At 12 weeks postinfection, all test mice had significant losses in body weight compared with those in controls (P < 0.05), a characteristic sign of bovine paratuberculosis. Tumor necrosis factor alpha was not detected in the serum. Histologic lesions were seen in the intestines, livers, and spleens of the animals in the orally inoculated test group after 26 weeks of infection. Our results suggest that the severe combined immunodeficient beige mouse may be a useful model for the investigation of paratuberculosis and cachexia and the evaluation of antimycobacterial drugs. 148 NAL Call. No.: 41.8 AM3A An experimental model for subclinical edema disease (Escherichia coli enterotoxemia) manifest as vascular necrosis in pigs. Kausche, F.M.; Dean, E.A.; Arp, L.H.; Samuel, J.E.; Moon, H.W. Schaumburg, Ill. : American Veterinary Medical Association; 1992 Mar. American journal of veterinary research v. 53 (3): p. 281-287; 1992 Mar. Includes references. Language: English Descriptors: Pigs; Edema; Latent infections; Disease models; Escherichia coli; Enterotoxemia; Animal models; Oral administration Abstract: An experimental model for subclinical edema disease was developed in weanling pigs. In multiple experiments, 3- week-old pigs were weaned, then inoculated intragastrically with 10(10) colony-forming units of an SLT-IIv-positive strain of Escherichia coli originally isolated from a pig with edema disease (principals). Control pigs were inoculated with a nonpathogenic E coli strain. Of 39 principals, 8 developed clinical edema disease within 14 days after inoculation. However, 20 of 21 principals that did not develop clinical signs of edema disease, but were submitted for necropsy examination at 14 days after inoculation, had characteristic vascular lesions of edema disease. Vascular lesions, found principally in ileum and brain, consisted of segmental necrosis of myocytes in the tunica media of small arteries and arterioles. None of the pigs inoculated with a nonpathogenic strain of E coli developed edema disease or vascular lesions. None of the principals necropsied at 2 days after inoculation had vascular lesions. Development of vascular lesions by 14 days after inoculation was used as the end point for detecting subclinical edema disease in the model. 149 NAL Call. No.: 41.8 J82 Experimental proliferative glomerulonephritis in the cat. Bishop, S.A.; Stokes, C.R.; Lucke, V.M. London : Academic Press; 1992 Jan. Journal of comparative pathology v. 106 (1): p. 49-60; 1992 Jan. Includes references. Language: English Descriptors: Cats; Glomerulonephritis; Disease models; Serum albumin; Intravenous injection; Symptoms; Animal models 150 NAL Call. No.: RB125.E9 Experimental surgery and physiology induced animal models of human disease. Swindle, M. Michael; Adams, Robert J. Baltimore : Williams & Wilkins,; 1988. x, 350 p. : ill. ; 27 cm. Includes bibliographies and index. Language: English Descriptors: Diseases; Animal models; Surgery, Experimental 151 NAL Call. No.: RB127.P34 The expression of a deafferentation syndrome in the Sprague- Dawley rat: effects of frontoparietal cortical lesions. Ovelmen-Levitt, J.; Young, J.N.; Rossitch, E. Jr; Nashold, B.S. Jr Amsterdam : Elsevier Science Publishers; 1991 Nov. Pain : the journal of the International Association for the Study of Pain v. 47 (2): p. 203-209; 1991 Nov. Includes references. Language: English Descriptors: Rats; Animal models; Lesions; Cerebral cortex; Nervous system diseases 152 NAL Call. No.: SF601.J65 Factors associated with failure of passive transfer of colostral antibodies in Standardbred foals. Clabough, D.L.; Levine, J.F.; Grant, G.L.; Conboy, H.S. Hagerstown, Md. : American College of Veterinary Medicine; 1991 Nov. Journal of veterinary internal medicine v. 5 (6): p. 335-340; 1991 Nov. Includes references. Language: English Descriptors: Foals; Maternal antibodies; Maternal immunity; Colostrum; Mares; Blood serum; Igg; Medical treatment; Animal models; Age 153 NAL Call. No.: 41.8 Ad9 Fasting hyperbilirubinemia in Bolivian squirrel monkeys with a Gilbert's-like syndrome. Cornelius, C.E. \u University of California, Davis, CA San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 127-147; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Hyperbilirubinemia; Fasting; Saimiri boliviensis; Animal models; Skin diseases; Nutrition; Bilirubin; Transferases 154 NAL Call. No.: 410.9 P94 Fasting hyperbilirubinemia in normal squirrel monkeys. Cornelius, C.E.; Freedland, R.A. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Feb. Laboratory animal science v. 42 (1): p. 35-37; 1992 Feb. Includes references. Language: English Descriptors: Saimiri sciureus; Hyperbilirubinemia; Fasting; Animal models; Bilirubin Abstract: The plasma of Bolivian squirrel monkeys, unlike that of Brazilian squirrel monkeys, is markedly yellow due to unconjugated hyperbilirubinemia after an overnight fast. The fasting hyperbilirubinemia in Bolivian squirrel monkeys is likely due to two mechanisms. First, a twofold increase in the bilirubin turnover/production rate occurs during a 24-hour fast. A second mechanism is the decreased hepatic conjugation potential for bilirubin due to the presence of a higher bilirubin UDP-glucuronosyltransferase (UDPGA)Km and a lower Vm; this results in higher steady-state plasma and hepatic bilirubin levels during a fast when hepatic UDP-glucuronic acid levels are low. The Bolivian squirrel monkey provides an excellent animal model for human Gilbert's syndrome type I in which to study rate-limiting mechanisms in the movement of bilirubin from plasma to bile. 155 NAL Call. No.: QP1.P4 Feeding conditions and estrous cycle of female rats under the activity-stress procedure from aspects of anorexia nervosa. Watanabe, K.; Hara, C.; Ogawa, N. Tarrytown, N.Y. : Pergamon Press; 1992 Apr. Physiology & behavior v. 51 (4): p. 827-832; 1992 Apr. Includes references. Language: English Descriptors: Anorexia nervosa; Food restriction; Feeding behavior; Activity; Stress; Food intake; Body weight; Estrous cycle; Mortality; Gastric ulcer; Histopathology; Animal models; Female animals; Rats Abstract: The present study investigated the application of female rats with activity stress as an animal model for anorexia nervosa. Young female rats were singly housed in activity-wheel cages with food-restricted schedule (2, 3, or 4 h of food availability per day) for 3 weeks. Estrous cycle, body, weight, food intake, and wheel revolution were recorded daily. Gastric pathology was also observed using the endoscopic technique. Rats that were subjected to either a 3- or 4-h feeding schedule exhibited the cessation of estrous cycle, loss of body weight, and suppression of food intake. These animals also showed a remarkable increase in running activity. However, they had no gastric lesions throughout the experimental period. On the contrary, the 2-h feeding schedule elicited severe gastric lesions and high mortality. The results suggest that behavioral and physiological changes of the young female rats with 3 or 4 h feeding share some symptoms of anorexia nervosa, although their anorexia is not self starvation. 156 NAL Call. No.: QR46.J6 Feeding trials of Listeria monocytogenes with a nonhuman primate model. Farber, J.M.; Daley, E.; Coates, F.; Beausoleil, N.; Fournier, J. Washington, D.C. : American Society for Microbiology; 1991 Nov. Journal of clinical microbiology v. 29 (11): p. 2606-2608; 1991 Nov. Includes references. Language: English Descriptors: Listeria monocytogenes; Foodborne diseases; Inoculum; Inoculum density; Infection; Symptoms; Disease models; Macaca fascicularis Abstract: One of the major unanswered questions regarding the presence of Listeria monocytogenes in foods is how many cells must be ingested in order to cause illness. To answer this question, studies were undertaken by using Macaca fascicularis (cynomolgus monkey) as an animal model. Healthy nonhuman primates were dosed with various concentrations of L. monocytogenes suspended in sterile whole milk. Final concentrations of 10(5), 10(7), and 10(9) total cells of the organism were used; a control was also included. Blood samples, as well as fecal and nasal specimens, were taken at various time intervals. Only animals that received 10(9) cells of L. monocytogenes became noticeably ill, with symptoms of septicemia, irritability, loss of appetite, and occasional diarrhea. Monkeys that received 10(7) and 10(9) cells shed L. monocytogenes in the feces for approximately 21 days. In monkeys that received the dose of 10(9) cells, severe lymphopenia and neutrophilia occurred within 48 h. In a separate trial, monkeys received Maalox to reduce the gastric acidity of the stomach. However, no substantial differences were observed between Maalox-treated and control monkeys. 157 NAL Call. No.: 41.8 P27 Feline mucopolysaccharidosis VII due to beta-glucuronidase deficiency. Gitzelmann, R.; Bosshard, N.U.; Superti-Furga, A.; Spycher, M.A.; Briner, J.; Wiesmann, U.; Lutz, H.; Litschi, B. Lawrence, Kan. : American College of Veterinary Pathologists; 1994 Jul. Veterinary pathology v. 31 (4): p. 435-443; 1994 Jul. Includes references. Language: English Descriptors: Cats; Beta-glucuronidase; Enzyme deficiencies; Mucopolysaccharidosis; Symptoms; Enzyme activity; Animal models; Case reports 158 NAL Call. No.: TX345.B74 Food allergy--role of mucosal immune regulation and oral tolerance: facts, fiction, and hypotheses. Strobel, S. San Diego : Academic Press, c1990-; 1993. Bristol-Myers Squibb/Mead Johnson nutrition symposia : [proceedings] v. 11: p. 335-364; 1993. Includes references. Language: English Descriptors: Food allergies; Immune response; Regulation; Intestinal mucosa; Oral administration; Human milk; Neonates; Autoimmunity; Antigens; Antibodies; T lymphocytes; Literature reviews Abstract: Physiological and immunological requirements for the acquisition of tolerance to dietary antigens (oral tolerance), based on experimental animal models and studies performed in human infants are discussed in this chapter. Tolerance in this context is defined as antigen-specific suppression of humoral antibody responses (IgM, IgG, IgE) and cell-mediated immunity after prior oral antigen exposure. 159 NAL Call. No.: 391.8 T662 Formate metabolism in young swine. Makar, A.B.; Tephly, T.R.; Sahin, G.; Osweiler, G. Orlando, Fla. : Academic Press; 1990 Sep01. Toxicology and applied pharmacology v. 105 (2): p. 315-320; 1990 Sep01. Includes references. Language: English Descriptors: Pigs; Formic acid; Formates (salts); Methanol; Metabolism; Folic acid; Toxicity Abstract: Formate generated from methanol metabolism in vivo is the chemical entity responsible for the development of the methanol toxicity syndrome in the monkey. Compared to rats, monkeys are in a state of folate deficiency. This leads to a decreased ability to dispose of formate generated leading to its accumulation and the subsequent development of the classic symptoms of methanol toxicity. Rats possess a more efficient folate system; therefore, they metabolize formate very readily and do not exhibit methanol toxicity symptoms. In this report, the hepatic folate content and the ability to handle a formate "load" were evaluated in another animal species, the pig. The results obtained indicate that the pig, compared to all other species studied, has extremely low levels of folates and very low levels of a key enzyme in the folate pathway, namely 10- formyl H4folate dehydrogenase. Also the pig's ability to dispose of formate was extremely limited and slower than that observed in rats or monkeys. These results suggest that the pig may be a suitable animal model for studying formate metabolism and possibly methanol toxicity. 160 NAL Call. No.: QP501.B64 Fulvic acid supplementation and selenium deficiency disturb the structural integrity of mouse skeletal tissue. Yang, C.; Niu, C.; Bodo, M.; Gabriel, E.; Notbohm, H.; Wolf, E.; Muller, P.K. London : The Biochemical Society; 1993 Feb01. The Biochemical journal v. 289 (pt.3): p. 829-835; 1993 Feb01. Includes references. Language: English Descriptors: Fulvic acids; Supplements; Selenium; Mineral deficiencies; Bone diseases; Collagen; Heat stability; Proline; Lysine; Bone strength Abstract: High concentrations of fulvic acid and selenium deficiency are the main causative factors of Kashin-Beck disease, an endemic, chronic and degenerative osteoarticular disorder found in China. In the search for an animal model of this disease, mice were exposed to these pathogenetic conditions for two generations and the collagen types from skin, bone and cartilage were analysed. The growth of the treated mice was slightly retarded, and the rate of reproduction was lower in animals maintained on a fulvic acid- supplemented and/or selenium-deficient diet. Irregular bone formation was seen by radiography and morphometry. Biochemical analysis indicated that lysine residues in collagen I from bone and in collagen II from cartilage were overmodified. The values of Hyl/(Hyl + Lys) in bone collagen alpha 1(I) chains from treated mice were about 0.434-0.484, i.e. substantially higher than that of the control (0.277). The values of this parameter for collagen II were 0.482 for control and 0.546-0.566 for treated mice. The melting temperature of collagen I from bones of treated mice was 1 degrees C lower than that of control collagen, indicating decreased thermal stability. The breakage point of the tibiae of treated mice occurred at a lower preload force than for controls, suggesting that the overmodified and thermally less stable collagen molecules are causally related to a lower mechanical strength of bones. 161 NAL Call. No.: QP141.A1N88 Gastrointestinal food allergy in childhood: current problems. Walker-Smith, J.A. Elmsford, N.Y. : Pergamon Press; 1992 Jan. Nutrition research v. 12 (1): p. 123-135; 1992 Jan. Literature review. Includes references. Language: English Descriptors: Food allergies; Gastroenteritis; Digestive tract; Infections; Animal models; Antigens; Intestinal absorption; Diagnosis; Children; Literature reviews Abstract: Two of the principal issues concerning gastrointestinal food allergy in infancy and early childhood are discussed. These are: The role of gastroenteritis, either in the initiation or unmasking of clinical manifestations of gastrointestinal food allergy. Secondly, the diagnostic criteria of gastrointestinal food allergy in childhood. The absolute first criterion for diagnosis must be a response to food elimination. The diagnostic approach is clearly defined for quick onset and slow onset cases. There are also a group of children who have mixed quick and slow onset symptoms. 162 NAL Call. No.: HV5285.A43 Genetic animal models. Crabble, J.C.; Phillips, T.J. Washington, D.C. : U.S. Department of Health and Human Services; 1990. Alcohol health and research world - National Institute on Alcohol Abuse and Alcoholism v. 14 (3): p. 179-180; 1990. Language: English Descriptors: U.S.A.; Animal experiments; Animal models; Genetic models; Alcoholism; Genetic regulation; Laboratory animals 163 NAL Call. No.: 44.8 J822 Genetic evaluation of somatic cell scores for United States dairy cattle. Schutz, M.M. Champaign, Ill. : American Dairy Science Association; 1994 Jul. Journal of dairy science v. 77 (7): p. 2113-2129; 1994 Jul. Includes references. Language: English Descriptors: U.S.A.; Cabt; Dairy cows; Somatic cell count; Bovine mastitis; Genetic gain; Milk yield; Selection criteria; Selection index; Genetic resistance; Breeding value; Heritability; Animal models; Genetic correlation; Breed differences; Literature reviews Abstract: Increases in milk yield from genetic selection may be accompanied by correlated increases in genetic susceptibility to clinical mastitis and somatic cells. Unlike clinical mastitis, somatic cell scores can be easily determined and recorded and are related to milk loss from subclinical mastitis. Selection against high somatic cell scores should decrease incidence of clinical mastitis and provide direct economic benefits through higher milk quality premiums. Genetic evaluation for lactation means of linear somatic cell scores has been implemented by USDA and parallels that for yield traits. Because additive genetics accounts for only about 10% of differences in somatic cell scores among cows, more information is needed for the same degree of confidence in genetic estimates as for yield. Only 80% of DHIA cows currently have somatic cell records. Thus, reliabilities of somatic cell evaluations are smaller than those for yield traits. Most progress in selection for lower somatic cell scores will come through sires of cows considered as bull dams. Somatic cell evaluations may best be reported through an economic index with a small amount of emphasis on somatic cell score relative to yield traits. Greater emphasis on somatic cell scores would decrease genetic gain in yield traits, which are economically more important. 164 NAL Call. No.: QP534.B56 Genetic influences on tissue deposition of aluminum in mice. Fosmire, G.J.; Focht, S.J.; McClearn, G.E. Totowa, N.J. : Humana Press; 1993 May. Biological trace element research v. 37 (2/3): p. 115-121; 1993 May. Includes references. Language: English Descriptors: Diet; Aluminum; Toxicity; Mineral metabolism; Tissues; Composition; Strain differences; Animal models; Disease models; Alzheimer's disease; Mice 165 NAL Call. No.: 410.9 P94 Genetic lipid storage disease with lysosomal acid lipase deficiency in rats. Yoshida, H.; Kuriyama, M. Cordova, Tenn. : American Association for Laboratory Animal Science; 1990 Sep. Laboratory animal science v. 40 (5): p. 486-489; 1990 Sep. Includes references. Language: English Descriptors: Human diseases; Disease models; Rats; Triacylglycerol lipase; Lysosomes; Symptoms; Pathology Abstract: We describe a new animal model of a genetic lipid storage disease analogous to human Wolman's disease. Affected Donryu rats, who inherited the disease in an autosomal recessive mode, manifested marked hepatosplenomegaly, lymph node enlargement, and thickened, dilated intestine. Morphologically, many characteristic foam cells were observed in livers and spleens. No adrenal calcification could be found in affected rats. Biochemical studies on spleen and liver tissues showed massive accumulation of esterified cholesterol and triglycerides, and deficiency of acid lipase for [14Cl- cholesteryl oleate. This animal model could contribute greatly to the clarification of the physiological and pathological roles of lysosomal acid lipase in the metabolism of lipoproteins and cholesterol, and of the pathogenesis of atherosclerosis. 166 NAL Call. No.: QR360.J6 Genetically engineered foot-and-mouth disease viruses with poly(C) tracts of two nucleotides are virulent in mice. Reider, E.; Bunch, T.; Brown, F.; Mason, P.W. Washington, D.C. : American Society for Microbiology; 1993 Sep. Journal of virology v. 67(9): p. 5139-5145; 1993 Sep. Includes references. Language: English Descriptors: Aphthovirus; Genetic engineering; Rna; Cytosine; Infectivity; Cell lines; Hamsters; Transfection; Deletions; Recombination; Cell culture; Virulence; Mice Abstract: To determine the role of the poly(C) tract found at the 5' end of the genome of foot-and-mouth disease virus, synthetic RNAs (in vitro transcripts) with poly(C) tracts of different lengths have been produced and evaluated. RNAs with poly(C) tracts of 35, 25, 16, 6, or 2 residues displayed similar specific infectivities in baby hamster kidney (BHK) cells. Viruses recovered from cells transfected with in vitro transcripts containing 6 to 35 Cs had properties similar to those of the wild-type virus in cell culture, and poly(C) tracts present in the synthetic RNA-derived viruses ranged from 75 to 140 bases in length. Viruses recovered from transcripts containing only two Cs showed very different properties. Specifically, viruses grew to much lower levels in cell culture and maintained a poly(C) tract of only two residues. The pool of viruses harvested from cells transfected with the synthetic C, RNA also contained a small amount of a virus with a 42-base deletion in the region of the poly(C) tract, which appeared to have arisen by recombination. Taken together, these data suggest that recombination provides the mechanism of poly(C) elongation and that viruses with poly(C) tracts over 75 bases in length have a selective advantage in cell culture. Interestingly, all of the in vitro transcript- derived viruses [including viruses with poly(C) tracts of only two residues] were equally virulent in mice, indicating that poly(C) tract length has no effect on virulence in this animal model. 167 NAL Call. No.: 410.9 P94 The gerbil, hamster, and guinea pig as rodent models for hyperlipidemia. Sullivan, M.P.; Cerda, J.J.; Robbins, F.L.; Burgin, C.W.; Beatty, R.J. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Dec. Laboratory animal science v. 43 (6): p. 575-578; 1993 Dec. Includes references. Language: English Descriptors: Hyperlipemia; Disease models; Animal models; Diets; Atherogenic diet; Gerbils; Hamsters; Guinea pigs; Cholesterol; Triacylglycerols Abstract: The purpose of this study was to compare the effects of a hyperlipidemic diet on three different rodent models to evaluate them on how their responses simulate human serum lipid diseases. Forty hamsters, 40 gerbils, and 20 guinea pigs were given either a chow diet or a modified high- fat, high-cholesterol diet (HF/HC) for 7 days. Food was withheld from half of the animals on each diet for 12 hours prior to collecting the blood for analysis of total cholesterol and triglyceride concentration. In all species, HF/HC feeding resulted in at least a 370% increase in total cholesterol concentration. Withholding food significantly decreased total cholesterol concentration in hamsters and gerbils fed HF/HC but had no effect on animals fed chow diet. Triglyceride concentrations were increased by the HF/HC in the hamster and the gerbil. As with total cholesterol, triglyceride concentration was decreased after food was withheld in these two animal groups. We suggest that the guinea pig is the most appropriate model for studying hypercholesterolemia because of its moderate plasma cholesterol response and normal triglyceride response to a HF/HC. We also suggest that the hamster is a good model for studying hypertriglyceridemia since increased serum triglyceride concentrations can be easily maintained on a HF/HC. 168 NAL Call. No.: 41.8 J82 Glycogen accumulation in the renal tubular cells of spontaneously occurring diabetic WBN/kob rats. Tsuchitani, M.; Kuroda, J.; Nagatani, M.; Miura, K.; Katoh, T.; Saegusa, T.; Narama, I.; Itakura, C. London : Academic Press; 1990 Feb. Journal of comparative pathology v. 102 (2): p. 179-190. ill; 1990 Feb. Includes references. Language: English Descriptors: Diabetes; Rats; Kidneys; Glycogen; Histopathology; Animal models; Disease models 169 NAL Call. No.: QP141.A1A63 Growth factors in milk as mediators of infant development. Donovan, S.M. \u University of Illinois, Urbana, IL; Odle, J. Palo Alto, Calif. : Annual Reviews Inc., c1981-; 1994 Jul. Annual review of nutrition v. 14: p. 147-167; 1994 Jul. Includes references. Language: English Descriptors: Human milk; Neonatal development; Epidermal growth factor; Insulin; Insulin-like growth factor; Relaxin; Peptides; Literature reviews Abstract: This review discusses findings on growth factors in milk and their potential roles in the neonate. The focus is on human milk, the human infant, and animal models used in research. The role of growth factors both in normal growth and development as well as their potential therapeutic role during recovery from intestinal injury is addressed. 170 NAL Call. No.: 41.8 Ad9 Gunn rat: a model for inherited deficiency of bilirubin glucuronidation. Chowdhury, J.R. \u Albert Einstein College of Medicine, Bronx, NY; Kondapalli, R.; Chowdhury, N.R. San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 149-173; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Liver diseases; Bilirubin; Animal models; Rats; Transferases; Bile pigments; Toxicity; Treatment 171 NAL Call. No.: QR360.A1J6 A hamster model of equine herpesvirus type 1 (EHV-1) infection; passive protection by monoclonal antibodies to EHV-1 glycoproteins 13, 14 and 17/18. Stokes, A.; Allen, G.P.; Pullen, L.A.; Murray, P.K. Reading : Society for General Microbiology; 1989 May. The Journal of general virology v. 70 (pt.5): p. 1173-1183; 1989 May. Includes references. Language: English Descriptors: Hamsters; Herpetoviridae; Glycoproteins; Monoclonal antibodies; Models 172 NAL Call. No.: RL79.H36 1994 Handbook of mouse mutations with skin and hair abnormalities animal models and biomedical tools.. Mouse mutations with skin and hair abnormalities Sundberg, John P. Boca Raton : CRC Press,; 1994. 544 p. : ill. ; 27 cm. (CRC series in dermatology). Includes bibliographical references and index. Language: English Descriptors: Skin; Hair; Mice as laboratory animals; Mice 173 NAL Call. No.: S451.P4P45 The hangover that lasts a lifetime. Ciresi, R. University Park, Pa. : Pennsylvania State University; 1991. PennState agriculture. p. 15-17; 1991. Language: English Descriptors: Fetal alcohol syndrome; Fetus; Animal models; Chicks 174 NAL Call. No.: 41.8 J82 Hepatic pathology of the colon carcinogen, azoxymethane, in Hanford-Moore miniature pigs. Wargovich, M.J.; Satterfield, W.; Price, R.E.; Stephens, L.C.; Coghlan, L. London : Academic Press; 1991 Oct. Journal of comparative pathology v. 105 (3): p. 271-278; 1991 Oct. Includes references. Language: English Descriptors: Miniature pigs; Animal models; Disease models; Colon; Azoxymethane; Carcinogens; Neoplasms; Toxicity; Liver; Histopathology 175 NAL Call. No.: 389.8 Z33 Hepatic selenium concentration in pigs with microangiopathy (mulberry heart disease)--an animal model for the study of oxidative damage. Korpela, H. Bern : Hogrefe & Huber Publishers; 1990. International journal for vitamin and nutrition research v. 60 (2): p. 156-159; 1990. Includes references. Language: English Descriptors: Diet; Mineral deficiencies; Selenium; Heart diseases; Pigs Abstract: The significance of selenium deficiency was investigated in pigs that died suddenly of microangiopathy (MAP, mulberry heart disease). Hepatic selenium concentration (mean +/- SD) in pigs with MAP (1.04 +/- 0.47 microgram/g dry weight) was lower than in healthy pigs (1.23 +/- 0.53 microgram/g). The lowest hepatic selenium values were found in pigs with MAP and in 22.2% of MAP pigs hepatic selenium concentration was below 0.5 microgram/g which reflects selenium deficiency. Thus, pigs with a low selenium status are at risk of MAR The low selenium status together with vitamin E deficiency increases oxidative stress and thus contributes to the development of oxidative damage. 176 NAL Call. No.: 41.8 P27 Hepatic storage of glycosaminoglycans in feline and canine models of mucopolysaccharidoses I, VI, and VII. Haskins, M.E.; Otis, E.J.; Hayden, J.E.; Jezyk, P.F.; Stramm, L. Lawrence, Kan. : American College of Veterinary Pathologists; 1992 Mar. Veterinary pathology v. 29 (2): p. 112-119; 1992 Mar. Includes references. Language: English Descriptors: Dogs; Cats; Animal models; Disease models; Mucopolysaccharidosis; Glycosaminoglycans; Liver; Hereditary diseases; Vacuoles 177 NAL Call. No.: 410.9 P94 Hereditary hydroenphrosis in C57BL/KsJ mice. Weide, L.G.; Lacy, P.E. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Oct. Laboratory animal science v. 41 (5): p. 415-418; 1991 Oct. Includes references. Language: English Descriptors: Mice; Nephrosis; Hereditary diseases; Incidence; Age differences; Kidneys Abstract: We sought to determine if the incidence of renal hydronephrosis in male C57BL/KsJ mice increased with age and if grossly normal kidneys would develop hydronephrosis over time. Spontaneous hydronephrosis was found incidentally in 32% of 234 male C57BL/KsJ mice killed as pancreas donors for islet transplantation experiments. The incidence of hydronephrosis increased with age; the incidence was 15% in 6- to 8-week-old mice, 52% in 8- to 10-week-old mice and 63% in 11- to 15-week- old mice (P < 0.001). Additional mice received islet isografts beneath the renal capsule. Only mice with grossly normal kidneys received islet grafts. These same kidneys were then re-examined when the graft recipients were killed at the end of the experiment and the incidence of hydronephrosis was determined. The conversion of normal kidneys to hydronephrotic kidneys increased with the time since islet transplantation. Kidneys re-examined less than 4 weeks since transplantation had only 5.8% new hydronephrosis, while those re-examined later than 4 weeks after transplantation had a new hydronephrosis incidence rate of 40% (P < 0.001). Our findings suggest that hydronephrosis is hereditary but not congenital, that it develops rapidly, and that it can complicate experiments using this strain. This may also represent a useful new animal model of progressive hydronephrosis. 178 NAL Call. No.: QP141.A1P46 Heterogeneity in sympathoadrenal activity in obesity: a function of type of obesity, nutrient effects, and regional responses. Young, J.B. Baton Rouge : Louisiana State University Press; 1992. Pennington Center nutrition series v. 2: p. 121-131; 1992. Includes references. Language: English Descriptors: Obesity; Nutrition physiology; Sympathetic nervous system; Energy metabolism; Epinephrine; Norepinephrine; Animal models; Literature reviews Abstract: Alterations in sympathetic nervous system activity, especially in brown fat, contribute to the regulation of energy expenditure in mammals. Adrenergic regulation of energy metabolism is believed to be abnormal in obesity, a phenomenon widely attributed to diminished sympathetic nervous system activity in brown fat. While reduced sympathetic nervous system activity in brown fat has been noted in many obese animals, it is not present in all. Furthermore, in one model of obesity, dogs or rodents fed lard-enriched diets, sympathetic nervous system activity is increased (elevated plasma norepinephrine levels and tissue norepinephrine turnover). Another abnormality noted with increasing frequency in both human and animal obesity is diminished adrenal epinephrine secretion, a process that is also influenced by nutrient intake. Although epinephrine is a potential regulator of energy metabolism in normal physiology, its role is incompletely understood. Moreover skeletal muscle, not brown fat, may be the principal site for thermic effects of epinephrine. Thus, while depressed sympathetic nervous system activity in brown fat may be sufficient, it is not a necessary explanation for obesity; adrenal medullary suppression may also contribute to the development of this condition. 179 NAL Call. No.: RC620.A1J6 Histidinemia: a biochemical variant or a disease?. Virmani, K.; Widhalm, K. Wilmington, NC : American College of Nutrition; 1993 Apr. Journal of the American College of Nutrition v. 12 (2): p. 115-124; 1993 Apr. Literature review. Includes references. Language: English Descriptors: Histidinemia; Amino acids; Metabolism; Genetic factors; Diet treatment; Diagnosis; Literature reviews; Maternal effects; Animal models Abstract: Histidinemia, first described by Ghadimi in 1961, is caused by a defect in histidase. The defect results in elevated urinary excretion of histidine and its transamination products, and in high blood histidine. Blood histidine levels in histidinemic patients range from 290 to 1420 micromolar (normal 70-120 micromolar). The clinical picture of histidinemia varies from complete normality to severe retardation, with many patients being asymptomatic. No correlation has been found between clinical and biochemical data. Most reported cases have been identified in newborn screening programs. Frequency of histidinemia ranges from 1 in 8000 (Japan) to 1 in 37,000 (Sweden). Histidinemia is inherited as an autosomal recessive trait. Maternal histidinemia is believed to be benign. Studies in animal models have shown similar metabolic changes in animals and humans, but clinical changes differ. Histidinemia may be treated with a low-histidine diet, which reduces elevated histidine levels, although in most cases no improvement of clinical symptoms has been observed. 180 NAL Call. No.: 41.8 J82 Histopathological and morphometrical comparison of granulomatous lesions in BALB/c and C3H/HeJ mice inoculated with Mycobacterium paratuberculosis. Tanaka, S.; Sato, M.; Taniguchi, T.; Yokomizo, Y. London : Academic Press; 1994 May. Journal of comparative pathology v. 110 (4): p. 381-388; 1994 May. Includes references. Language: English Descriptors: Mycobacterium paratuberculosis; Histopathology; Susceptibility; Mice; Strain differences; Animal models; Genes; Disease course; Granuloma; Liver; Spleen 181 NAL Call. No.: QL55.A1L3 Housing, breeding and selecting chickens of the Obese strain (OS) with spontaneous autoimmune thyroiditis. Dietrich, H.M. London : Royal Society of Medicine Services; 1989 Oct. Laboratory animals v. 23 (4): p. 345-352. ill; 1989 Oct. Includes references. Language: English Descriptors: Fowls; Thyroid diseases; Autoimmune diseases; Hereditary diseases; Disease models; Chicken housing; Animal breeding; Selection methods Abstract: A management programme is described for a small colony of Obese strain (OS) chickens afflicted with spontaneous hereditary thyroiditis. Animals of this White Leghorn fine are used as an animal model for Hashimoto's thyroiditis of man to study possible mechanisms of autoimmunity in general and organ-specific autoimmune diseases in particular. Due to the severe mononuclear cell infiltration of the thyroid glands, OS chickens show symptoms of hypothyroidism, including small body size, subcutaneous and abdominal fat deposits, long silky feathers, small combs and wattles, cold sensitivity, low fertility and poor hatchability. Successful breeding of this line, especially in a small population, can therefore be done only if rigid precautions are taken in aspects of animal care. The selection of breeding stock, the principal requirements for adequate housing and food, the artificial insemination procedure, and recommendations for collecting and incubating chicken eggs are reported in detail. Precautions necessary during the incubation of fertilized eggs, and fertility and hatchability are reported. During the hatching period several specific features must be considered. The important role of staff involved in a small chicken breeding unit is emphasized. 182 NAL Call. No.: RC620.A1J6 The human intestinal response to enteral nutrients: a review. Jackson, W.D.; Grand, R.J. New York, N.Y. : John Wiley & Sons; 1991 Oct. Journal of the American College of Nutrition v. 10 (5): p. 500-509; 1991 Oct. Literature review. Includes references. Language: English Descriptors: Malnutrition; Gastrointestinal diseases; Literature reviews; Enteral feeding; Starvation; Parenteral feeding; Digestive tract mucosa; Nutrient requirements; Nutritional assessment Abstract: This review identifies the factors which influence mucosal integrity during enteral nutrition. These include biliary and pancreatic secretions, trophic influences of endocrine and gastrointestinal polypeptides, intestinal blood flow, and innervation. Fiber, bacterial fermentation products, purines, and glutamine are potential essential nutrients which may not be provided by parenteral nutrition. However, contrary to experience in animal models, the specific advantages of intraluminal delivery of nutrients for the maintenance of mucosal integrity and structure remain unproven in the human. Current evidence in the human suggests that changes in small bowel structure and function when enteral nutrients are excluded are minor and rapidly reversible as long as general nutritional status is maintained. 183 NAL Call. No.: 500 N21P Hyperinsulinemia induces a reversible impairment in insulin receptor function leading to diabetes in the sand rat model on non-insulin-dependent diabetes mellitus. Kanety, H.; Moshe, S.; Shafrir, E.; Lunenfeld, B.; Karasik, A. Washington, D.C. : National Academy of Sciences,; 1994 Mar01. Proceedings of the National Academy of Sciences of the United States of America v. 91 (5): p. 1853-1857; 1994 Mar01. Includes references. Language: English Descriptors: Psammomys obesus; Diabetes mellitus; Experimental diabetes; Hyperinsulinemia; Insulin; Hormone receptors; Liver; Muscles; Protein kinase; Animal models; Overfeeding Abstract: The insulin receptor was evaluated at different disease stages in the sand rat (Psammomys obesus), a model for nutrition-induced diabetes. Nondiabetic sand rats showed markedly low receptor number in liver compared with albino rats. Their receptor had an intact tyrosine kinase activity but a higher Km, for ATP in the phosphorylation reaction of exogenous substrates. The initial effects of overeating (i.e., development of hyperinsulinemia without hyperglycemia) were associated in the sand rat with a dramatic decrease in in vitro and in vivo insulin-induced receptor tyrosine kinase activity in both liver and muscle. In muscle, this coincided with a decrease in receptor number and an increase in basal tyrosine kinase activity. Similar changes were observed upon development of hyperinsulinemia with hyperglycemia. Upon recovery from the diabetic state by diet restriction, the impaired receptor kinase activation was corrected. Complete restoration occurred only in animals that fully recovered from the diabetic state and became normoinsulinemic. These observations indicate that loss and gain of receptor tyrosine kinase activity were dependent on insulin levels. Thus, overeating may lead to the development of hyperinsulinemia through ineffective extraction of excess insulin by the scarce liver receptors. Hyperinsulinemia, in turn, causes a reversible reduction in receptor kinase activity, leading to insulin resistance. This sequence of events may be relevant to diet-related changes in human non-insulin-dependent diabetes mellitus. 184 NAL Call. No.: 500 N21P Hyperuricemia and urate nephropathy in urate oxidase-deficient mice. Wu, X.; Wakamiya, M.; Vaishnav, S.; Geske, R.; Montgomery, C. Jr; Jones, P.; Bradley, A.; Caskey, C.T. Washington, D.C. : National Academy of Sciences,; 1994 Jan18. Proceedings of the National Academy of Sciences of the United States of America v. 91 (2): p. 742-746; 1994 Jan18. Includes references. Language: English Descriptors: Mice; Oxidoreductases; Uric acid; Targeted mutagenesis; Homologous recombination; Structural genes; Embryonic stem cells; Mutants; Hyperuricemia; Nephropathy; Animal models; Disease models Abstract: Urate oxidase, or uricase (EC 1.7.3.3), is a purine metabolic enzyme that catalyzes the conversion of uric acid to allantoin in most mammals except humans and certain other primates. The loss of urate oxidase in the human during primate evolution predisposes man to hyperuricemia, a metabolic disturbance that can lead to gouty arthritis and renal stones. To create a mouse model for hyperuricemia and gout, and to address the question of whether urate oxidase is essential in lower mammalian species, we have disrupted the urate oxidase gene in the mouse by homologous recombination in embryonic stem cells. Unlike the human situation, urate oxidase deficiency in mice causes pronounced hyperuricemia and urate nephropathy. More than half of the mutant mice died before 4 weeks of age, indicating that urate oxidase is essential in mice. These mutant mice may also serve as animal models for hyperuricemia and its related nephropathy in humans. 185 NAL Call. No.: 500 N21P Identification and prevalence of genetic defect that causes leukocyte adhesion deficiency in Holstein cattle. Shuster, D.E.; Kehrli, M.E. Jr; Ackermann, M.R.; Gilbert, R.O. Washington, D.C. : The Academy; 1992 Oct01. Proceedings of the National Academy of Sciences of the United States of America v. 89 (19): p. 9225-9229. ill; 1992 Oct01. Includes references. Language: English Descriptors: Calves; Holstein-friesian; Animal models; Bovine leukosis; Genetic defects; Identification; Incidence; Mutations; Nucleotide sequences; Screening; Bulls; Culling Abstract: Two point mutations were identified within the gene encoding bovine CD18 in a Holstein calf afflicted with leukocyte adhesion deficiency (LAD). One mutation causes an aspartic acid to glycine substitution at amino acid 128 (D128G) in the highly conserved extracellular region of this adhesion glycoprotein, a region where several mutations have been found to cause human LAD. The other mutation is silent. Twenty calves with clinical symptoms of LAD were tested, and all were homozygous for the D128G allele. In addition, two calves homozygous for the D128G allele were identified during widespread DNA testing, and both were subsequently found to exhibit symptoms of LAD. The carrier frequency for the D128G allele among Holstein cattle in the United States is approximately 15% among bulls and 6% among cows. This mutation is also prevalent among Holstein cattle throughout the world, placing this disorder among the most common genetic diseases known in animal agriculture. All cattle with the mutant allele are related to one bull, who through the use of artificial insemination sired many calves in the 1950s and 1960s. The organization of the dairy industry and the diagnostic test described herein will enable nearly complete eradication of bovine LAD within 1 year. These results also demonstrate that bovine LAD is genetically homologous and phenotypically similar to human LAD, thus providing a useful animal model for studies of LAD and beta 2 integrin function. 186 NAL Call. No.: 41.8 AM3A Immune response of cattle to Haemophilus somnus lipid A- protein conjugate vaccine and efficacy in a mouse abortion model. Inzana, T.J.; Todd, J. Schaumburg, Ill. : American Veterinary Medical Association; 1992 Feb. American journal of veterinary research v. 53 (2): p. 175-179; 1992 Feb. Includes references. Language: English Descriptors: Cattle; Antibody formation; Haemophilus somnus; Vaccines; Lipids; Abortion; Animal models; Mice Abstract: Immunogenicity of the lipid A component of Haemophilus somnus lipooligosaccharide in cattle and mice was examined after purification, detoxification, and covalent conjugation to a protein carrier. After 2 inoculations, a substantial antibody response was induced in most cattle to lipid A and the protein carrier. To determine whether antibodies to lipid A would be protective, 5 X 10(7) colony- forming units of H somnus strain 649 were administered IV to endotoxin-responsive (C3H/HEN) mice. In one study, 8 of 13 C3H/HEN mice aborted when inoculated. In contrast, abortion did not result when mice were inoculated with the same dose of an isolate of H somnus normally found in the prepuce or with the rough mutant Escherichia coli J5. In addition, endotoxin- nonresponsive (C3H/HeJ) mice were significantly (P = 0.03) more resistant to abortion by strain 649 than were C3H/HeN mice, but inoculated C3H/HeN mice were only slightly more resistant to H somnus abortion, compared with control mice. Although a large antibody response to lipid A was detected, there was no significant difference in the immunized group between mice that aborted and mice that delivered normally. Thus, lipooligosaccharide and other properties of virulent H somnus strains may contribute to abortion in mice. 187 NAL Call. No.: RC267.I53 1988 Immune-deficient animals in experimental medicine. Wu, Bing-quan,_1930-; Zheng, Jie International Workshop on Immune-Deficient Animals 6th : 1988 : Peking, China. Basel ; New York : Karger,; 1989. xiii, 361 p. : ill. ; 25 cm. Includes bibliographical references and index. Language: English Descriptors: Cancer; Animal models; Congresses; Immunological deficiency syndromes; Animal models; Congresses; Mice; Immunology; Congresses; Rats; Immunology; Congresses 188 NAL Call. No.: RC606.I45 Immunodeficient rodents a guide to their immunobiology, husbandry, and use. Institute of Laboratory Animal Resources (U.S.), Committee on Immunologically Compromised Rodents Washington, D.C. : National Academy Press,; 1989. x, 246 p. : ill. ; 24 cm. Includes index. Bibliography: p. 165-211. Language: English Descriptors: Immunological deficiency syndromes; Animal models; Rodents; Immunology; Rodents as laboratory animals 189 NAL Call. No.: 41.8 P27 Immunohistochemical, ultrastructural, and hormonal studies on the endocrine pancreas of voles (Microtus arvalis) with monosodium aspartate-induced diabetes. Sasaki, M.; Arai, T.; Usui, T.; Oki, Y. Lawrence, Kan. : American College of Veterinary Pathologists; 1991 Nov. Veterinary pathology v. 28 (6): p. 497-505; 1991 Nov. Includes references. Language: English Descriptors: Diabetes mellitus; Hormones; Ultrastructure; Immunohistochemistry; Endocrine system; Pancreas islets; Microtus arvalis; Histopathology; Animal models; Disease models 190 NAL Call. No.: QR46.J6 Immunomagnetic separation and DNA hybridization for detection of enterotoxigenic Escherichia coli in a piglet model. Lund, A.; Wasteson, Y.; Olsvik, O. Washington, D.C. : American Society for Microbiology; 1991 Oct. Journal of clinical microbiology v. 29 (10): p. 2259-2262; 1991 Oct. Includes references. Language: English Descriptors: Norway; Piglets; Diarrhea; Feces; Digesta; Escherichia coli; Enterotoxins; Bacterial antigens; Fimbriae; Genes; Dna hybridization; Magnetic separation; Immunodiagnosis Abstract: Enterotoxigenic Escherichia coli (ETEC) strains were detected by stool blot hybridization assays using different oligonucleotide probes for the colonization fimbrial antigen F4, heat-stable enterotoxin I (ST I), and heat-labile enterotoxin (LT I) genes. Forty-eight fecal samples and seven samples of intestinal content from ETEC-challenged newborn piglets were processed in two ways: (i) by direct inoculation of bacterial suspension onto nylon membranes overlaying blood agar and (ii) by immunomagnetic enrichment of F4+ ETEC using magnetic beads coated with F4 monoclonal antibodies before inoculation onto nylon membranes. In samples obtained from nondiarrheic piglets pre- and postchallenge, E. coli genes for F4, ST I, and LT I could be detected only after immunomagnetic enrichment. No difference between the two methods in detection of these E. coli genes was observed when stool blots from diarrheic piglets were examined. By using magnetic separation, it was easy to decrease background bacterial flora, intestinal cells, and fecal debris and thus produce purer specimens. The method evaluated in this animal model appeared simple and quick and increased the sensitivity of detection of ETEC strains 100-fold compared with the direct stool blot hybridization assays. Prior bacterial isolation and identification were not necessary. 191 NAL Call. No.: QP141.H78 The immunopathology of zinc deficiency in humans and rodents. A possible role for programmed cell death. Fraker, P.J.; King, L.E.; Garvy, B.A.; Medina, C.A. New York ; London, Plenum; 1993. Human nutrition : a comprehensive treatise v. 8: p. 267-283; 1993. In the series analytic: Nutrition and immunology / edited by D.M. Klurfeld. Includes references. Language: English Descriptors: Zinc; Mineral deficiencies; Animal models; Immunopathology; Cells; Nutrition research; Death; Thymus gland; Endocrine glands; B lymphocytes; Phagocytes; Protein energy malnutrition; Bone marrow; Glucocorticoids; Elderly; Nutritional state; Nutrition physiology; Species differences; Rats; Adults; Literature reviews Abstract: This chapter explores whether or not the zinc deficient rat appears to be a useful model for humans and whether there are common patterns of immune defects observed between the species. Studies are reviewed on the efficacy of zinc supplementation on the immune status of the mildly deficient elderly. 192 NAL Call. No.: QP901.A33 Impaired glucose-induced insulin secretion: studies in animal models with spontaneous NIDDM. Ostenson, C.G.; Khan, A.; Efendic, S. New York : Plenum Press, 1967-; 1993. Advances in experimental medicine and biology v. 334: p. 1-11; 1993. In the series analytic: New concepts in the pathogenesis of NIDDM / edited by C.G. Ostenson, S. Efendic, and M. Vranic. Proceedings of the "Second Toronto-Stockholm Symposium on Perspectives in Diabetes Research," September 13-16, 1992, Stockholm, Sweden. Includes references. Language: English Descriptors: Diabetes mellitus; Insulin secretion; Glucose; Animal models 193 NAL Call. No.: 389.8 B773 Impaired T lymphocyte immune response in vitamin A depleted rats and chicks. Friedman, A.; Sklan, D. Cambridge : Cambridge University Press; 1989 Sep. The British journal of nutrition v. 62 (2): p. 439-449; 1989 Sep. Includes references. Language: English Descriptors: Diet; Vitamin deficiencies; Retinol; T lymphocytes; Immune response; Rats; Chicks Abstract: Vitamin A deficiency results in decreased immune responses; the objective of the present study was to investigate the involvement of T lymphocytes in the depression of immune responses resulting from vitamin A depletion. This objective was achieved by evaluating antigen-specific T lymphocyte proliferative responses in vitro as vitamin A depletion developed. The evaluation was performed in both rat and chick to examine the generality of immune effects due to vitamin A depletion. Our findings show that vitamin A depletion led to severe impairment of T lymphocyte activity in both animal models, and that this was directly related to the vitamin A status in both species. Immune response impairment was found to precede other manifestations of vitamin A deficiency, and was rapidly corrected by feeding retinyl acetate boluses. This implied a possible regulatory, rather than constitutive, role of vitamin A in immune responsiveness. 194 NAL Call. No.: 381 J824 In vivo correction of low density lipoprotein receptor deficiency in the Watanabe heritable hyperlipidemic rabbit with recombinant adenoviruses. Kozarsky, K.F.; McKinley, D.R.; Austin, L.L.; Raper, S.E.; Stratford-Perricaudet, L.D.; Wilson, J.M. Baltimore, Md. : American Society for Biochemistry and Molecular Biology; 1994 May06. The Journal of biological chemistry v. 269 (18): p. 13695-13702; 1994 May06. Includes references. Language: English Descriptors: Rabbits; Hyperlipemia; Hypercholesterolemia; Animal models; Low density lipoprotein; Receptors; Deficiency; Hereditary diseases; Gene therapy; Gene transfer; Complementary DNA; Recombinant DNA; Adenoviridae; Gene expression; Reporter genes; Beta-galactosidase; Liver cells; Promoters; Cholesterol metabolism Abstract: A rabbit animal model of the human disease familial hypercholesterolemia (FH), which is the result of low density lipoprotein (LDL) receptor deficiency, was used to develop an in vivo approach to gene therapy based on recombinant adenoviruses. Recombinant, replication-defective adenoviruses expressing the lacZ gene under the control of different promoters were infused into the portal circulation of New Zealand White (NZW) rabbits. Expression of lacz could be obtained in virtually all hepatocytes within 3 days post- infusion, but was undetectable by 3 weeks. This was not associated with liver pathology.An LDL receptor expressing adenovirus was constructed using the most active promoter and was infused into the portal vein of rabbits deficient in LDL receptor. Analysis of liver tissues harvested 3 days after virus infusion demonstrated human LDL receptor protein in the majority of hepatocytes that exceeded the levels found in human liver by at least 10-fold. Transgene expression was stable for 7-10 days and diminished to undetectable levels within 3 weeks. Infusion of LDL receptor expressing virus led to substantial reductions in serum cholesterol that returned to base line within 3 weeks; this acute reduction in serum cholesterol was associated with accumulations of lipid in hepatocytes. The development of neutralizing antibodies to the recombinant adenovirus markedly diminished the effectiveness of a second dose. These studies illustrate the advantages of recombinant adenoviruses for the treatment of liver metabolic diseases and define issues, such as viral genome instability and blocking immune response, that need to be overcome before the promise of this technology can be fully realized. 195 NAL Call. No.: QR360.A1J6 In vivo detection of metabolic changes in a mouse model of scrapie using nuclear magnetic resonance spectroscopy. Bell, J.D.; Cox, I.J.; Williams, S.C.R.; Belton, P.S.; McConnell, I.; Hope, J. Reading : Society for General Microbiology; 1991 Oct. The Journal of general virology v. 72 (pt.10): p. 2419-2423; 1991 Oct. Includes references. Language: English Descriptors: Scrapie; Mice; Metabolites; Nuclear magnetic resonance spectroscopy; Membranes; Proteins; Animal models Abstract: In vivo proton nuclear magnetic resonance (NMR) spectroscopy studies of scrapie in a mouse model have shown the appearance of an abnormal peak in the brain early in the incubation period. This abnormal peak was detected weeks before the detection of a protease-resistant form of a membrane protein and vacuolar histopathology in vitro, and several months before clinical signs, and the signal increased in intensity as the disease progressed. In the chronic stage of the disease, a reduction in N-acetyl aspartate levels was observed using in vivo and in vitro proton NMR spectroscopy. 196 NAL Call. No.: QL55.A1L3 Influence of chronic oestrogen treatment on severity of hydronephrosis in inbred DDD mice. Mannen, H.; Tsuji, S.; Goto, N. London : Royal Society of Medicine Services; 1993 Apr. Laboratory animals v. 27 (2): p. 124-130; 1993 Apr. Includes references. Language: English Descriptors: Mice; Estrogens; Urination disorders; Animal models Abstract: It has been reported that mice treated chronically with oestrogen (oestradiol propionate) increase their bladder urine volume. Since inbred DDD mice, particularly male DDD mice, lack a protective mechanism against vesicoureteral reflux (VUR), chronic oestrogen treatment may increase the pressure in the renal pelvis and lead to severe hydronephrosis. The present studies were carried out to confirm this hypothesis. Results of a least-squares analysis of variance showed that the severity of hydronephrosis was more severe after treatment with high doses of oestrogen (1.0 and 5.0 mg/kg/week) in entire and castrated male DDD mice. Hydroureter was also observed in the same groups. Intra- vesicular pressure was 7 to 12 cmH2O higher in mice of these groups than in control DDD mice. High doses of oestrogen had no effect on the kidneys of C57BL/6 mice which showed normal protection against VUR, though it increased bladder urine volume. These findings support the hypothesis that hydronephrosis in DDD mice is caused by an incomplete protective mechanism against VUR. 197 NAL Call. No.: 410.9 P94 Influenza virus infections and immunity: a review of human and animal models. Renegar, K.B. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Jun. Laboratory animal science v. 42 (3): p. 222-232; 1992 Jun. Literature review. Includes references. Language: English Descriptors: Influenzavirus; Influenza; Animal models; Immune response; Man; Domestic animals; Experimental infection; Vaccination; Literature reviews Abstract: Studies of the pathogenesis of influenza infection have involved the extensive use of animal models. The development of the current concepts of immunity to influenza and of the contribution the secretory immune system makes toward the protection of mucosal surfaces against influenza infection would have been impossible without this use of animals. The pathology, and clinical signs of influenza infection in both natural and experimental hosts, the advantages and disadvantages of the most common experimental influenza infection models, and the contribution of animal models to the understanding of local and systemic immunity to influenza infection are discussed. 198 NAL Call. No.: RA1190.F8 Inhibition of hen brain acetylcholinesterase and neurotoxic esterase by chloropyrifos in vivo and kinetics of inhibition by chlorpyrifos oxon in vitro: application to assessment of neuropathic risk. Richardson, R.J.; Moore, T.B.; Kayyali, U.S.; Fowke, J.H.; Randall, J.C. Orlando, Fla. : Academic Press; 1993 Apr. Fundamental and applied toxicology : official journal of the Society of Toxicology v. 20 (3): p. 273-279; 1993 Apr. Includes references. Language: English Descriptors: Chlorpyrifos; Metabolites; Toxicity; Nervous system diseases; Dosage effects; Enzyme activity; Acetylcholinesterase; Esterases; Inhibition; Kinetics; Brain; In vitro; Hens; Lethal dose Abstract: Chlorpyrifos (CPS, O,O-diethyl 3,5, 6-trichloro-2- pyridyl phosphorothionate; Dursban) is a widely used broad- spectrum organophosphorus (OP) insecticide. Because some OP compounds can cause a sensory-motor distal axonopathy called OP compound-induced delayed neurotoxicity (OPIDN), CPS has been evaluated for this paralytic effect. Early studies of the neurotoxicity of CPS in young and adult hens reported reversible leg weakness but failed to detect OPIDN. More recently, a human case of mild OPIDN was reported to result from ingestion of a massive dose (about 300 mg/kg) in a suicide attempt. Subsequent experiments in adult hens (the currently accepted animal model of choice for studies of OPIDN) showed that doses of CPS in excess of the LD50 in atropine-treated animals inhibited brain neurotoxic esterase (NTE) and produced mild to moderate ataxia. Considering the extensive use of CPS and its demonstrated potential for causing OPIDN at supralethal doses, additional data are needed to enable quantitative estimates to be made of the neuropathic risk of this compound. Previous work has shown that the ability of OP insecticides to cause acute cholinergic toxicity versus OPIDN can be predicted from their relative tendency to inhibit the intended target, acetylcholines (AChE), versus the putative neuropathic target, NTE, in brain tissue. The present study was designed to clarify the magnitude of neuropathic risk associated with CPS exposures by measuring hen brain AChE and NTE inhibition following dosing in vivo and determining the bimolecular rate constant of inhibition (ki) for each enzyme by the active metabolite, CPS oxon (CPO), in vitro. CPS administered to atropine-treated adult hens at 0, 75, 150, and 300 mg/kg po in corn oil produced mean values for brain AChE inhibition 4 days after dosing of 0, 58, 75, and 86%. respectively, and mean values for brain NTE inhibition of 0, 21. 40, and 77%, respectively. Only the high dose (six times the unprotected LD50 in hens) pro 199 NAL Call. No.: QR1.I57 Inoculation of barrier-born pigs with Helicobacter pylori: a useful animal model for gastritis type B. Engstrand, L.; Gustavsson, S.; Jorgensen, A.; Schwan, A.; Scheynius, A. Washington, D.C. : American Society for Microbiology; 1990 Jun. Infection and immunity v. 58 (6): p. 1763-1768. ill; 1990 Jun. Includes references. Language: English Descriptors: Bacteria; Pigs; Models; Gastritis; Inoculation 200 NAL Call. No.: 500 N21P Insulin-induced activation of glycerol-3-phosphate acyltransferase by a chiro-inositol-containing insulin mediator is defective in adipocytes of insulin-resistant, type II diabetic, Goto-Kakizaki rats. Farese, R.V.; Standaert, M.L.; Yamada, K.; Huang, L.C.; Zhang, C.; Cooper, D.R.; Wang, Z.; Yang, Y.; Suzuki, S.; Toyota, T.; Larner, J. Washington, D.C. : National Academy of Sciences,; 1994 Nov08. Proceedings of the National Academy of Sciences of the United States of America v. 91 (23): p. 11040-11044; 1994 Nov08. Includes references. Language: English Descriptors: Rats; Diabetes mellitus; Glycerol-3-phosphate acyltransferase; Enzyme activity; Insulin; Regulation; Adipocytes; Hormonal control; Inositol phosphates; Animal models; Phosphatidylinositols; Experimental diabetes Abstract: Type II diabetic Goto-Kakizaki (GK) rats were insulin-resistant in euglycemic-hyperinsulinemic clamp studies. We therefore examined insulin signaling systems in control Wistar and diabetic GK rats. Glycerol-3-phosphate acyltransferase (G3PAT), which is activated by headgroup mediators released from glycosyl-phosphatidylinositol (GPI). was activated by insulin in intact and cell-free adipocyte preparations of control, but not diabetic, rats. A specific chiro-inositol-containing inositol phosphoglycan (IPG) mediator, prepared from beef liver, bypassed this defect and comparably activated G3PAT in cell-free adipocyte preparations of both diabetic GK and control rats. A myo-inositol- containing IPG mediator did not activate G3PAT. Relative to control adipocytes, labeling of GPI by [3H]glucosamine was diminished by 50% and insulin failed to stimulate GPI hydrolysis in GK adipocytes. In contrast to GPI-dependent G3PAT activation, insulin-stimulated hexose transport was intact in adipocytes and soleus and gastrocnemius muscles of the GK rat, as was insulin-induced activation of mitogen- activated protein kinase and protein kinase C. We conclude that (i) chiro-inositol-containing IPG mediator activates G3PAT during insulin action, (ii) diabetic GK rats have a defect in synthesizing or releasing functional chiro-inositol- containing IPG, and (iii) defective IPG-regulated intracellular glucose metabolism contributes importantly to insulin resistance in diabetic GK rats. 201 NAL Call. No.: QR360.A1J6 Interactions between equine herpesvirus type 1 and equine herpesvirus type 4: T cell responses in a murine infection model. Azmi, M.; Field, H.J. Reading : Society for General Microbiology; 1993 Nov. The Journal of general virology v. 74 (pt.11): p. 2339-2345; 1993 Nov. Includes references. Language: English Descriptors: Equine herpesvirus; Immune response; T lymphocytes; Animal models; Mice Abstract: Interactions involving the immune responses to equine herpesvirus types 1 and 4 (EHV-1 and EHV-4) were studied in a murine infection model. When mice were inoculated intranasally with EHV-1, virus replication occurred in the respiratory tract and clinical signs were produced. In contrast, mice that were similarly inoculated with EHV-4 produced no evidence of virus replication and showed no clinical signs. When mice that had been inoculated with live EHV-4 were challenged 1 month later with EHV-1 they were partially protected. Although clinical signs were apparent on reinfection, virus replication in the respiratory tract was reduced in these mice compared with control mice that had not been previously immunized. Mice primed with heat-inactivated EHV-4, however, were not so protected. Live EHV-4-primed mice developed very low levels of antibody to EHV-1 and the humoral response could not account for this protection. However, the infected mice did give a strong delayed-type hypersensitivity reaction in a skin test using either EHV-1 or EHV-4 antigen. Spleen cells from EHV-4-primed donors provided a source of immune cells, including T cells which were used for transfer to recipient mice which were then challenged with EHV-1. The cells were protective; there was a reduction of virus replication on challenge with EHV-1 which correlated with the number of cells transferred. Modulation of the protective effect of primed cell populations was tested after depletion in vivo by means of complement-mediated lysis. The depletion of CD4-bearing cells produced the least effect on the protection afforded by cell transfer. In contrast, depletion of CD8-bearing cells markedly reduced the protection in recipients. EHV-1 and EHV-4 are widespread in horses and cross-infections are common. These results gained from a murine model indicate that important interactions occur at the level of T cell immunity. between the two virus types which warrant further investigation in the natural host. 202 NAL Call. No.: 447.8 AM3 Intraluminal and intracellular phases of fat adsorption are impaired in essential fatty acid deficiency. Levy, E.; Garofalo, C.; Thibault, L.; Dionne, S.; Daoust, L.; Lepage, G.; Roy, C.C. Bethesda, Md. : American Physiological Society; 1992 Feb. American journal of physiology v. 262 (2,pt.1): p. G319-G326; 1992 Feb. Includes references. Language: English Descriptors: Essential fatty acids; Fat deficiencies; Triacylglycerols; Lipoproteins; Nutrient transport; Fat absorption; Intestinal absorption Abstract: The structure and function of enterocyte membranes are particularly sensitive to the degree of fatty acid saturation. The objective of the present study was to assess intestinal fat transport in essential fatty acid (EFA)- deficient animal models. Both the digestive and absorptive phases leading to the formation and the secretion of triglyceride (TG)-rich lipoproteins were investigated. After an intraduodenal fat infusion, the percentage increase of plasma TG over fasting values was examined over a period of 4 h in two groups of control and EFA-deficient rats. Lower values at 1 and 2 h (P < 0.05) were observed in EFA deficient rats, suggesting fat malabsorption. Likewise, postprandial chylomicronemia was diminished. In a separate group of rats, EFA deficiency was associated with reduced TG and chylomicron- TG transport into lymph. Although pancreatic lipase activity did not change (47.1 vs. 46.2 micromoles free fatty acids.mg protein-1.h-1), bile flow was decreased over the 8-h period of collection. Concomitantly, a significant decline (nmol.min-1.g liver-1, P < 0.05) was discernible in the biliary secretory rate of bile salts (14.09 +/- 2.13 vs. 35.09 +/- 3.73), phospholipids (7.01 +/- 0.61 vs. 11.79 +/- 1.65) and cholesterol (0.19 +/-0.01 vs. 0.83 +/- 0.06). In vitro studies, utilizing everted sacs incubated with mixed micelles, revealed that EFA-deficient jejunal segments of rats incorporated and esterified less [14C]oleic acid (21 and 32%, respectively). Moreover, the synthesis and secretion of TG- rich lipoproteins were found markedly reduced in mouse jejunal explant cultures. We conclude that EFA deficiency modifies both the intraluminal and intracellular phases of fat absorption. 203 NAL Call. No.: 389.8 J82 Iron and folate utilization in reproducing swine and their progeny. O'Connor, D.L.; Picciano, M.F.; Roos, M.A.; Easter, R.A. Bethesda, Md. : American Institute of Nutrition; 1989 Dec. The Journal of nutrition v. 119 (12): p. 1984-1991; 1989 Dec. Includes references. Language: English Descriptors: Pigs; Pregnancy; Lactation; Diet; Iron; Folic acid; Metabolism Abstract: The purpose of this investigation was to assess the usefulness of maternal and neonatal swine as animal models for studying iron (Fe) and folate nutrition during reproduction and growth. Sows (n = 18) were fed a purified diet containing 0.6 mg folate/kg diet and either 25 (Fe-) or 125 (Fe+) mg iron/kg diet throughout gestation and lactation. Litters were culled to eight on d 2 of lactation and four piglets/litter were given an intramuscular injection of iron dextran (100 mg/kg body wt). Plasma and red blood cell folate concentrations among all sows decreased (>50%) after conception (P < 0.001). Plasma folate concentration of Fe- sows was 47% and 69% of Fe+ sows on d 7 and 21 of lactation, respectively (P < 0.05). All sows secreted milk that contained low levels of folate (12-36 nmol/l) and was devoid of long- chain folylpolyglutamates While mean milk folate concentration significantly decreased after d 1 of lactation among Fe- sows, no such decrease was observed in milk from Fe+ sows (P < 0.05). Liver folate concentration was significantly reduced in piglets nursed by Fe- sows and given intramuscular iron dextran. It is concluded that there is an increased dietary requirement for folate and iron during reproduction in swine, and that current recommended amounts of folate (0.6 mg/kg diet) and iron (80 mg/kg diet) may be underestimates of requirements for reproduction. Further, results show that iron nutrition may alter folate utilization in maternal and neonatal swine. 204 NAL Call. No.: QP141.A1P72 Is vitamin E supplementation a useful agent in AIDS therapy?. Wang, Y.; Watson, R.R. Tarrytown, N.Y. : Pergamon Press; 1993 Oct. Progress in food & nutrition science v. 17 (4): p. 351-375; 1993 Oct. Includes references. Language: English Descriptors: Vitamin e; Acquired immune deficiency syndrome; Vitamin supplements; Immune response; Oxidation; Stress; Cytokines; Human immunodeficiency virus; Nervous system diseases; Antioxidants; Neutrophils; Nutritional state; Literature reviews Abstract: Acquired immune deficiency syndrome (AIDS) is a clinical disorder caused by a retrovirus infection, representing the end point in a progressive sequence of immunosuppressive changes. The literature is briefly summarized as to immunological, nutritional and other pathological modifications caused by AIDS, and properties of immunoenhancing, anti-oxidant and undernutrition-restoration of vitamin E supplementation. All these abnormalities in AIDS are similar to those that are stimulated or restored by intake of high doses of vitamin E. The drawbacks of pharmacological therapy like zidovudine (AZT), e.g. deleterious toxic side effects, inability to improve the immune dysfunctions and undernutrition initiated by the retrovirus infection, and finding of AZT-resistant HIV strains, necessitate new strategies for the clinical trials of novel therapies to treat AIDS with the existing medical therapies. Low toxicity nutritional agents with immunoenhancing and antioxidant activities like vitamin E may help to normalize retrovirus- induced immune dysfunctions, undernutrition and other pathological symptoms, thereby retarding the progression of the disease to AIDS. To address this vitamin E therapeutic role in HIV-positive individuals. This paper presents a review of vitamin E-related therapeutic roles in animals and humans, thereby showing why vitamin E supplementation could be used as a useful therapeutic agent in human AIDS therapy. Since there is a paucity of information available regarding the nutritional therapy in AIDS individuals, our purpose is to provide evidence from animal models or humans of the potential therapeutic role of vitamin E supplementation in the treatment of AIDS individuals. 205 NAL Call. No.: 385 J822 Isolation and localization of the 120 kDa protein in the liver of genetically obese Zucker rats. Maeda, H.; Kasahara, K. Tokyo : Japanese Biochemical Society; 1994 Jan. The Journal of biochemistry v. 115 (1): p. 37-40; 1994 Jan. Includes references. Language: English Descriptors: Rats; Obesity; Liver; Animal proteins; Cytosol; Lipogenesis; Lipid metabolism; Animal models Abstract: The genetically obese Zucker rat is a well- characterized model of early-onset human obesity. The 120 kDa protein was recently found in the liver cytosol of obese Zucker rats at levels higher than that in lean Zucker rats. We isolated this protein using precipitation with ammonium sulfate, DEAE-Sephacel chromatography, and preparative polyacrylamide gel electrophoresis; the product showed a single band on SDS-polyacrylamide gel electrophoresis. Immunoblotting analysis revealed that the 120 kDa protein was predominantly localized in the liver cytosol of obese Zucker rats. The amount of this protein in lean Zucker rats was less than one-fifth of that found in obese Zucker rats. Further, there were only trace amounts of this protein in the lung tissues, and no detectable amount in other tissues, such as kidney, epididymal adipose tissue, brain, spleen, skeletal muscle, or serum, in either strain of rat. These data suggest that the 120 kDa protein contributes to the abnormal lipid metabolism in obese Zucker rats. 206 NAL Call. No.: 410.9 P94 Isotype-specific rabbit antibodies against chinchilla immunoglobulins G, M, and A. Konietzko, S.; Koskela, M.; Erdmann, G.; Giebink, G.S. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Jun. Laboratory animal science v. 42 (3): p. 302-306; 1992 Jun. Includes references. Language: English Descriptors: Chinchillas; Isolation; Igg; Igm; Iga; Blood serum; Milk; Isotypes; Rabbits; Antibodies; Immune serum Abstract: Chinchillas have become a preferred animal model for studying otitis media, and are also useful in studying insulin release, gastrin physiology, intestinal infection, and hepatocellular pathophysiology. Immunopathologic studies in the model, however, have been limited by absence of specific antibody reagents against chinchilla immunoglobulins. We describe a method for preparing isotype-specific rabbit antibodies against the heavy-chain components of chinchilla immunoglobulins G, M, and A. Chromatographic techniques were used to isolate chinchilla immunoglobulins from serum and breast milk; heavy-chain fractions were isolated and used as antigens to produce isotype-specific antibodies in New Zealand White rabbits. Enzyme-linked immunosorbent assay of these antisera disclosed anti-light chain cross-reactivity, which was removed by affinity chromatography. The isolation and affinity purification techniques were highly reproducible. The availability of these reagents should greatly enhance the utility of the chinchilla in modeling human disease. 207 NAL Call. No.: QL55.A1I43 Jcr:LA-corpulent rat: a strain with spontaneous vascular and myocardial disease. Russell, J.C.; Koeslag, D.G. Washington, D.C. : Institute of Laboratory Animal Resources, National Research Council; 1990. I.L.A.R. news v. 32 (3): p. 27-32; 1990. Includes references. Language: English Descriptors: Rats; Animal models; Vascular diseases; Heart diseases 208 NAL Call. No.: RC628.N48 1987 The LA/N-corpulent rat as a model of atherosclerosis. Russell, J.C.; Heisler, O.R.; Amy, R.M. Bethesda, Md. : National Institutes of Health; 1988. New models of genetically obese rats for studies in diabetes, heart disease, and complications of obesity : NIH workshop, June 18-19, 1987, summaries of workshop papers and current bibliography. p. 163-165; 1988. Language: English Descriptors: Atherosclerosis; Animal models; Rats 209 NAL Call. No.: QL55.A1L33 Large animal models of human disease. Lewis, S.M.; Carraway, J.H. New York, N.Y. : Nature Publishing Company; 1992 Jan. Lab animal v. 21 (1): p. 22-29; 1992 Jan. Includes references. Language: English Descriptors: Animal models; Human diseases 210 NAL Call. No.: QH442.B5 Lipoproteins and heart disease. Breslow, J. New York, N.Y. : Nature Publishing,; 1994 Apr. Bio/technology v. 12 (4): p. 365-370; 1994 Apr. Language: English Descriptors: Mice; Transgenic animals; Apolipoproteins; Structural genes; Molecular genetics; Experimental atherosclerosis; Animal models; Very low density lipoprotein 211 NAL Call. No.: 442.8 B5236 Liver and muscle-fat type glucose transporter gene expression in obese and diabetic rats. Yamamoto, T.; Fukumoto, H.; Koh, G.; Yano, H.; Yasuda, K.; Masuda, K.; Ikeda, H.; Imura, H.; Seino, Y. Duluth, Minn. : Academic Press; 1991 Mar29. Biochemical and biophysical research communications v. 175 (3): p. 995-1002. ill; 1991 Mar29. Includes references. Language: English Descriptors: Obesity; Diabetes mellitus; Carbohydrate metabolism; Glucose; Insulin; Resistance; Genes; Gene expression; Messenger RNA; Liver; Skeletal muscle; Rats Abstract: In order to investigate the regulation of glucose transporter gene expression in the altered metabolic conditions of obesity and diabetes, we have measured mRNA levels encoding GLUT2 in the liver and GLUT4 in the gastrocnemius muscle from various insulin resistant animal models, including Zucker fatty, Wistar fatty, and streptozocin(STZ)-treated diabetic rats. Northern blot analysis revealed that GLUT2 mRNA levels were significantly (P<0.001) elevated in 14 wk Zucker fatty and Wistar fatty rats relative to lean littermates but were similar in these two groups at 5 wk of age. Furthermore, there was significant increase (P<0.01) in GLUT2 mRNA levels in STZ diabetic rats at 3 wk after treatment. GLUT4 mRNA levels were not significantly different between control and insulin resistant rats in all animal models. These results indicate that neither hyperinsulinemia nor hyperglycemia affects GLUT4 mRNA levels in the muscle. However, GLUT2 mRNA levels in the liver were elevated in obesity and diabetes, although this regulatory event occurred independently from circulating insulin or glucose concentrations. 212 NAL Call. No.: RC660.A1D53 Low-protein diets in renal disease. Zeller, K.R. Alexandria, Va. : American Diabetes Association; 1991 Sep. Diabetes care v. 14 (9): p. 856-866; 1991 Sep. Literature review. Includes references. Language: English Descriptors: Kidney diseases; Morbidity; Mortality; Protein intake; Animal models; Protein secretion; Renal function; Renal failure; Literature reviews; Man Abstract: End-stage renal disease is a major cause of morbidity and mortality in the U.S. population and a significant contributor to national health-care expenditures. In recent years, a growing body of literature has accumulated from studies in animals and humans to suggest that dietary protein restriction can significantly retard the progression of chronic renal insufficiency. This article reviews the relevant literature and outlines the questions that remain for future investigation. 213 NAL Call. No.: 410.9 P94 Lymphoblastic lymphoma in a colony of N:NIH (S)-bg-nu-xid mice. Waggie, K.S.; Wu-Owens, J.; Hollifield, V.; Hansen, C.T. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Aug. Laboratory animal science v. 42 (4): p. 375-377; 1992 Aug. Includes references. Language: English Descriptors: Mice; Lymphoma Abstract: During a 1-year period, 28 animals from a breeding colony of N:NIH(S)-bg-nu-xid mice were discovered to have rapidly enlarging subcutaneous swellings in the ventral, cervical, and axillary regions. Five of the mice also had hind limb paresis. Twenty-two of the mice were heterozygous nude females, five were homozygous nude males, and one was a homozygous nude female. All of the above mice were homo- or hemizygous for the beige and X-linked immunodeficiency mutations. The average age of the mice was 8.3 months. Generalized enlargement of the peripheral and internal lymph nodes was present at the time of necropsy examination. Other lesions commonly noted at necropsy included splenomegaly (15 mice), pale and thickened ventral lumbar spinal musculature (11 mice), and opaque, thickened meninges of the brain (10 mice). Histologic examination consistently disclosed infiltrates of neoplastic lymphoblasts in multiple tissues including lymph nodes, spleen, bone marrow, and meninges of the brain and spinal cord. The cells were positive for IgG on immunofluorescent staining, suggesting that the tumors were of B cell origin. The neoplasms observed in these mice have several similarities to tumors found in immunodeficient humans, suggesting that these mice may serve as useful animal models of lymphoma. 214 NAL Call. No.: RC628.T697 1992 Marked caloric restriction and organ response in normal-weight and obese experimental animals. Young, E.A. New York : Guilford Press; 1992. Treatment of the seriously obese patient / edited by Thomas A. Wadden, Theodore B. VanItallie ; foreward by Per Bjorntorp. p. 107-135; 1992. Includes references. Language: English Descriptors: Calorie-restricted diets; Metabolic studies; Nutrition physiology; Animal models 215 NAL Call. No.: 389.9 N953 The mechanisms and treatment of weight loss in cancer. Fearon, K.C.H. Cambridge : Cambridge University Press; 1992 Aug. Proceedings of the Nutrition Society v. 51 (2): p. 251-265; 1992 Aug. The Sir David Cuthbertson Medal lecture 1991 presented at the University of Leeds, November 1991. Includes references. Language: English Descriptors: Carcinoma; Cachexia; Anorexia; Protein metabolism; Cytokines; Diet treatment; Energy metabolism; Drug therapy; Literature reviews Abstract: In this lecture, the author examines the metabolic disturbance, specifically weight loss, in patients with cancer. It covers: changes in body composition; the role of anorexia; animal models of cancer cachexia; the role of cytokines; protein metabolism; tumor energy metabolism; and dietary and pharmacological manipulation of tumor growth. 216 NAL Call. No.: TX551.N87 Mechanisms of food intolerances: development and use of experimental animal models. Miller, K.; Nicklin, S. London : Taylor & Francis; 1988. Nutritional and toxicological aspects of food processing : proceedings of an interntional symposium held at the Istituto Superiore di Sanita, Rome, Italy, 14-16 April 1987 / edited by R. Walker and E. Quattrucci. p. 351-364; 1988. Includes references. Language: English Descriptors: Food intolerance; Animal experiments 217 NAL Call. No.: 448.8 M56 Membrane fluidity and sodium transport by renal membranes from dogs with spontaneous idiopathic Fanconi syndrome. Hsu, B.Y.L.; McNamara, P.D.; Mahoney, S.G.; Fenstermacher, E.A.; Rea, C.T.; Bovee, K.C.; Segal, S. Orlando, Fla. : W.B. Saunders Co; 1992 Mar. Metabolism: clinical and experimental v. 41 (3): p. 253-259; 1992 Mar. Includes references. Language: English Descriptors: Dogs; Fanconi syndrome; Kidneys; Membranes; Sodium; Nutrient uptake; Nutrient transport; Animal models 218 NAL Call. No.: 448.8 M56 Metabolic abnormalities of the hyperglycemic obese Zucker rat. McCaleb, M.L.; Sredy, J. Philadelphia, Pa. : W.B. Saunders Co; 1992 May. Metabolism: clinical and experimental v. 41 (5): p. 522-525; 1992 May. Includes references. Language: English Descriptors: Diabetes mellitus; Hyperglycemia; Obesity; Metabolism; Physiopathology; Animal models; Rats 219 NAL Call. No.: 41.8 Ad9 Metabolic fatty liver of ruminants. Bruss, M.L. \u University of California, Davis, CA San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 417-449; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Cows; Sheep; Fatty liver; Liver; Triacylglycerols; Lipid metabolism; Long chain fatty acids; Animal models; Literature reviews 220 NAL Call. No.: QL55.A1L3 A method for hyperthermic treatment of mouse skin. Gragtmans, N.J.; Jevcak, J.J.; Mitchel, R.E.J.; Morrison, D.P.; McCann, R.A.; Murphy, J.W. London : Royal Society of Medicine Services; 1992 Apr. Laboratory animals v. 26 (2): p. 122-126; 1992 Apr. Includes references. Language: English Descriptors: Mice; Skin; Animal models; Disease models; Hyperthermia; Carcinogenesis; Promoters; Carcinogens Abstract: The Sencar mouse skin system is a recognized model for tumour initiation, promotion and progression. The current interest in the effect of hyperthermia on this multi-stage tumorigenesis model prompted the need for a technique to accurately heat a section of dorsal skin of a large number of mice for 30 min per heat treatment. In the technique described, experimental groups of 25 female Sencar mice were treated at 7-8 weeks of age under general methoxyflurane anaesthesia. Treatment consisted of the application of initiating and/or promoting agents with or without hyperthermia. For hyperthermic skin treatments, each group of mice was placed onto a platform in a water bath so that the dorsal skin of the mice was in contact with 44 degrees C temperature controlled water. 221 NAL Call. No.: QP43.M47 Methods in animal physiology. Deyl, Zdenek; Zicha, Joseph Boca Raton, Fla. : CRC Press,; 1989. 438 p. : ill. ; 26 cm. Includes bibliographies and index. Language: English Descriptors: Physiology, Experimental; Methodology; Pathology, Experimental; Methodology; Diseases; Animal models 222 NAL Call. No.: QP141.A1J54 Methyl deficiency, DNA methylation, and cancer: studies on the reversibility of the effects of a lipotrope-deficient diet. Christman, J.K.; Chen, M.L.; Sheikhnejad, G.; Dizik, M.; Abileah, S.; Wainfan, E. Newton, Mass. : Butterworth-Heinemann; 1993 Dec. The Journal of nutritional biochemistry v. 4 (12): p. 672-680; 1993 Dec. Includes references. Language: English Descriptors: Lipotropic factors; Deficiency; Carcinoma; Diet; Dna methylation; Carcinogenesis; Gene expression; Animal models; Rats Abstract: Methylation of C residues in CpG sites in the regulatory, regions of a wide variety of genes has been linked to silencing of their expression. During normal mammalian development, loss of methylation at specific sites accompanies tissue-specific activation of genes. Overall decreases in the level of DNA methylation and alterations in the pattern of methylation of specific genes are also closely linked to tumor development in humans and other mammals. Dietary methyl deficiency sufficient to cause hepatocarcinogenesis in male rats induces profound and rapid changes in the morphology and metabolic activity of liver cells. As we have previously reported, these changes include a decrease in the overall level of DNA methylation and alternations in the patterns of methylation and levels of transcripts of specific growth- related genes. These alterations persist as long as the rats are maintained on a methyl-deficient diet. The starting hypothesis for the studies summarized here is that methyl deficiency induced changes in liver cells that persist, even when dietary sources of methyl groups are restored, are more likely to be critical for establishment of neoplasia than those that are reversible. We find that loss of methylation at specific sites in liver DNA persists for at least 9 weeks after restoration of methionine, choline, folate, and vitamin B12 to the diet of rats previously deprived of these nutrients for 4 weeks. Other molecular changes are reversed in less than 3 weeks. This suggests that exposure of rats to alternating periods of dietary methyl deficiency and sufficiency may provide an experimental model for determining whether persistent alterations in methylation of growth regulatory genes allow affected hepatocytes to escape constraints on cell division because they respond to growth stimuli differently than cells in which the genes are normally methylated. 223 NAL Call. No.: 500 N484 The microepidemiology of wasting syndrome, a common link to diarrheal disease, cancer, rabies, animal models of AIDS, and HIV-AIDS (HAIDS): the feline leukemia virus and rabies virus models. Tshikuka, J.G.; Torres-Anjel, M.J.; Blenden, D.C.; Elliott, S.C. New York, N.Y. : The Academy; 1992. Annals of the New York Academy of Sciences v. 653: p. 274-296. ill; 1992. In the series analytic: Tropical veterinary medicine: current issues and perspectives / edited by J.C. Williams, K.M. Kocan, and E.P.J. Gibbs. Literature review. Includes references. Language: English Descriptors: Acquired immune deficiency syndrome; Epidemiology; Human immunodeficiency virus; Disease models; Feline oncovirus; Rabies virus; Literature reviews 224 NAL Call. No.: 442.9 SO1 Minimum requirements of n-3 and n-6 essential fatty acids for the function of the central nervous system and for the prevention of chronic disease. Okuyama, H. Baltimore, Md. : Williams & Wilkins; 1992 Jun. Proceedings of the Society for Experimental Biology and Medicine v. 200 (2): p. 174-176; 1992 Jun. Proceedings of a "Conference on Molecular and Comparative Nutrition," July 22-24, 1991, National Institutes of Health, Bethesda, Maryland. Includes references. Language: English Descriptors: Linoleic acid; Linolenic acid; Safflower oil; Perilla; Plant oils; Nutrition; Animal behavior; Animal physiology; Central nervous system; Diseases; Disease prevention; Animal models; Rats; Mice Abstract: General behavioral patterns of rats or mice fed 5 wt% safflower oil (75% linolenate [n-6] and < 0.1% alpha- linolenate [n-3]) for two generations were significantly different from those of animals fed 5 wt% perilla oil (15% n-6 and 55% n-3). Also, brightness-discrimination learning ability and retinal function were higher in the perilla group than in the group fed 5 wt% soybean oil (53% n-6 and 4.7% n-3) or safflower oil, indicating that the requirement of n-3 for the maximum responses of the nervous system is above 0.6 en% when there is 6.8 en% linoleate n-6. Perilla oil has been found to be beneficial for the suppression of carcinogenesis, allergic hyperreactivity, thrombotic tendency, apoplexy, hypertension, and aging in animals, as compared with soybean oil and safflower oil. These results are against a lipid peroxide theory of aging, carcinogenesis, and chronic diseases. Animal experiments and epidemiological studies lead to a recommendation that the intake of n-6 should be decreased to as low as 2-4 en% and that of n-3 be increased to levels higher than linoleate n-6 for the prevention of chronic diseases prevailing in the industrialized countries. 225 NAL Call. No.: QD341.A2N8 Mitochondrial genome expression in a mutant strain of D. subobscura, an animal model for large scale mtDNA deletion. Beziat, F.; Morel, F.; Volz-Lingenhol, A.; Saint Paul, N.; Alziari, S. Oxford : IRL Press; 1993 Feb11. Nucleic acids research v. 21 (3): p. 387-392; 1993 Feb11. Includes references. Language: English Descriptors: Drosophila subobscura; Mitochondrial DNA; Deletions; Mitochondrial genetics; Genomes; Transcription; Gene expression; Messenger RNA; Genes; Transfer RNA; Structural genes; Nadh dehydrogenase; Cytochrome b Abstract: A mitochondrial mutant strain of D. subobscura has two mitochondrial genome populations (heteroplasmy): the first (20-30% of the population, 15.9 kb) is the same as could be found in the wild type; the second (70-80% of the population, 11 kb) has lost by deletion several genes coding for complex I and III subunits, and four tRNAs. In human pathology, this kind of mutation has been correlated with severe diseases such as the Kearns-Sayre syndrome, but the mutant strain does not seem to be affected by the mutation. Studies reported here show that: a) Transcripts from genes not concerned by the mutation are present at the same level in both strains. b) In contrast, transcript concentrations from genes involved in the deletion are significantly decreased (30-50%) in the mutant. c) Deleted DNA was expressed as shown by the detection of the fusion transcript. d) The mtDNA/nuc.DNA ratio is 1.5 times higher in the mutant strain than in the wild type. The mutation leads to change in the transcript level equilibrium. The apparent innocuousness of the mutation may suggest some post-transcriptional compensation mechanisms. This drosophila strain is an interesting model to study the consequence of this type of mitochondrial genome deletion. 226 NAL Call. No.: 410.9 P94 A model of postprandial hyperinsulinemia in miniature swine. Weingard, K.W. Cordova, Tenn. : American Association for Laboratory Animal Science; 1989 Sep. Laboratory animal science v. 39 (5): p. 394-399; 1989 Sep. Includes references. Language: English Descriptors: Pigs; Hyperinsulinemia; Insulin; Diets; Disease models; Atherosclerosis Abstract: This report describes a new animal model of postprandial hyperinsulinemia (PPH) in adult miniature swine that consume a diet simulating that of affluent Western societies. Two progressive levels of PPH were induced experimentally by injecting subcutaneously low and high doses of purified porcine insuline without causing acute detrimental clinical effects or significant biological effects on total serum cholesterol, sodium and potassium concentrations, mean arterial blood pressure, or heart rate. Physiologic postprandial increments in total serum triglyceride concentrations were inhibited by experimentally-induced PPH. With this model, the in vivo effects of homologous PPH can be studied in a dose-responsive manner. Areas of potential research use of this model include study of the chronic effects of PPH on lipoprotein metabolism, the development of atherosclerosis and diabetes mellitus, and the association with regional body fat distribution and metabolism. 227 NAL Call. No.: 447.8 AM3 Model of spontaneous obesity in aging male Wistar rats. Newby, F.D.; DiGirolamo, M.; Cotsonis, G.A.; Kutner, M.H. Bethesda, Md. : American Physiological Society; 1990 Dec. American journal of physiology v. 259 (6,pt.2): p. R1117- R1125; 1990 Dec. Includes references. Language: English Descriptors: Obesity; Adipose tissue; Growth; Adipocytes; Morphology; Body fat; Body weight; Animal models; Rats; Aging; Male animals Abstract: We analyzed retrospectively data from 148 chow-fed male Wistar rats killed between the age of 6 wk and 2 yr while varying in body weight from 136 to 917 g. The purpose of this study was to clarify the relationship of body weight and body lipid content with the composition and cellularity of the epididymal and retroperitoneal fat depots. A positive linear association was found between body weight and body water or fat-free dry residue, whereas total body lipid exhibited a curvilinear relationship with body weight. The weight of the epididymal pads was linearly related to body weight but not to body lipid. In contrast, retroperitoneal pad weight was exponentially related to body weight and paralleled total body lipid. A strong linear correlation was found between total body lipid and weight (r = 0.959) or depot lipid content (r = 0.967) of the retroperitoneal fat pads. In this rat model of aging and spontaneous obesity, significant regional differences exist in adipose depot composition and cellularity. A practical outcome of this study is a simple and accurate prediction of body lipid content from the gravimetric determination of the retroperitoneal fat depots. 228 NAL Call. No.: QL55.A1I43 Modeling in biomedical research: an assessment of current and potential approaches. Washington, D.C. : Institute of Laboratory Animal Resources, National Research Council; 1990. I.L.A.R. news v. 32 (2): p. 2-3; 1990. Language: English Descriptors: Animal models; Disease models; Cardiovascular diseases; Diabetes mellitus; Animal experiments; Computer simulation; Medical research 229 NAL Call. No.: 41.8 J82 Morphological changes associated with furazolidone-induced cardiomyopathy: effects of digoxin and propranolol. Gwathmey, J.K. London : Academic Press; 1991 Jan. Journal of comparative pathology v. 104 (1): p. 33-45; 1991 Jan. Includes references. Language: English Descriptors: Animal models; Disease models; Cardiomyopathy; Poults; Furazolidone; Histopathology; Digoxin; Propranolol; Muscular hypertrophy 230 NAL Call. No.: RC280.L5M67 Mouse liver carcinogenesis mechanisms and species comparisons : proceedings of a symposium held in Austin, Texas, November 30-December 3, 1988. Stevenson, Donald E. M.D. Anderson Cancer Center, Science-Park Research Division New York : A.R. Liss,; 1989. xix, 444 p. : ill. ; 24 cm. (Progress in clinical and biological research ; v. 331). Conference hosted by the Science Park-Research Division of the University of Texas M.D. Anderson Cancer Center in Smithville, Tex. Includes bibliographical references. Language: English Descriptors: Liver; Tumors; Congresses; Cancer; Animal models; Congresses; Carcinogenicity testing; Congresses; Carcinogenesis; Congresses; Mice; Diseases; Congresses 231 NAL Call. No.: 410.9 P94 Mouse model for disseminated Trichosporon beigelii infection. Bannatyne, R.M.; Fong, I.W.; Cheng, P.; Capellan, J.M. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Apr. Laboratory animal science v. 42 (2): p. 168-169; 1992 Apr. Includes references. Language: English Descriptors: Mice; Animal models; Trichosporon beigelii; Mycoses; Experimental infection 232 NAL Call. No.: 410.9 P94 Mouse models of short- and long-term foreign body in the urinary bladder: analogies to the bladder segment of urinary catheters. Johnson, D.E.; Lockatell, C.V.; Hall-Craggs, M.; Warren, J.W. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Oct. Laboratory animal science v. 41 (5): p. 451-455; 1991 Oct. Includes references. Language: English Descriptors: Mice; Animal models; Bladder; Catheters; Foreign bodies; Bacterial diseases; Experiments; Long term experiments Abstract: Catheter-associated bacteriuria is the most common infection occurring in hospitals, where urethral catheters are generally in place for a few days, and in nursing homes, where catheters may be in place for months or years. We developed murine models with intrabladder urinary catheters for studying complications of bacteriuria in short- and long-term catheterization. In the short-term model, a catheter segment was inserted transurethrally and lay free within the bladder lumen. Half of the animals expelled segments during a 2-to-7- day period, durations similar to catheterizations in hospitalized patients. For studies of long-term catheter use, the catheter segment was secured within the bladder by a single suture for up to 12 months. Antibiotics administered for 7 days after catheter placement and housing mice in cages with wire screen floors reduced spontaneous bacteriuria to an acceptably low incidence rate of only 7%. Proteus mirabilis bacteriuria of high concentration provoked the same complications that are common in patients with long-term catheters: acute pyelonephritis, chronic renal inflammation, and struvite stone formation. These models allow inoculation of the bacteria of interest and are suitable for studies of short- and long-term foreign body-associated bacteriuria and its complications. 233 NAL Call. No.: 410.9 P94 The muskrat in biomedical research. Doyle, R.E.; Panneton, W.M.; Vogler, G.A.; Romeo, J.P.; Watson, B.J.; Higgins, B. Cordova, Tenn. : American Association for Laboratory Animal Science; 1988 Dec. Laboratory animal science v. 38 (6): p. 667-674. ill; 1988 Dec. Includes references. Language: English Descriptors: Muskrats; Animal husbandry; Animal health; Handling; Quarantine; Medical research; Animal experiments Abstract: Muskrats are aquatic rodents of moderate size which are plentiful throughout North America, but are not used commonly in the laboratory. Recently, we tested the feasibility of muskrats as experimental models and have found them to be acquired and cared for easily in conventional laboratory animal facilities. Some of their natural characteristics and diseases are described. The husbandry techniques that we used are presented and form a base for the preparation of future guidelines for the maintenance and use of feral animals in research. The results of some initial experiments testing the muskrat's utility for investigations of cardiorespiratory control mechanisms also are presented. Our data show that even anesthetized muskrats possess brisk and dramatic cardiovascular and respiratory reflexes. Our findings that their brains possess the cytoarchitectural and myeloarchitectural features comparable to other mammals, combined with their relative uniformity in size, has allowed us to locate specific neuronal loci stereotaxically. We suggest that the muskrat be considered as an experimental animal model for studies of the neural control of cardiorespiratory systems. 234 NAL Call. No.: 41.8 P27 Mycobacterium paratuberculosis monossociated nude mice as a paratuberculosis model. Hamilton, H.L.; Cooley, A.J.; Adams, J.L.; Czuprynski, C.J. Lawrence, Kan. : American College of Veterinary Pathologists; 1991 Mar. Veterinary pathology v. 28 (2): p. 146-155; 1991 Mar. Includes references. Language: English Descriptors: Mice; Mycobacterium paratuberculosis; Disease models; Peptides; Necrosis; Animal models 235 NAL Call. No.: QP141.A1P72 Neuroendocrine alterations in iron deficiency. Beard, J.L. Elmsford, N.Y. : Pergamon Press; 1990. Progress in food and nutrition science v. 14 (1): p. 45-80. charts; 1990. Literature review. Includes 141 references. Language: English Descriptors: Iron; Mineral deficiencies; Mineral metabolism; Neurophysiology; Neurosecretory systems; Temperature; Catecholamines; Animal experiments; Human nutrition research Abstract: A model of iron metabolism has been used for several years and suggests that the deleterious consequences of iron deficiency occur only after depletion of body iron stores. The biochemical consequences of iron deficiency have been adequately reviewed by others and will be covered only briefly here. This review will focus on those effects of iron deficiency on neuroendocrine processes. Out of necessity, many of these observations are derived from the rat as a animal model and are limited in breadth and depth of investigation. The rat model has been reasonable for many studies of iron metabolism and tissue biochemistry, but serious concerns can and should be raised when neuroendocrine relationships are being investigated. Nonetheless, strong parallels have been observed between effects of iron deficiency anemia in humans and the rat model especially with regard to thyroid metabolism and catecholamines. The discrepancies may reflect the greater severity of the deficiency generated in the rat as well as the rate of development of the deficiency. 236 NAL Call. No.: QR360.A1J6 Neurological abnromalities associated with feline immunodeficiency virus infection. Phillips, T.R.; Prospero-Garcia, O.; Puaoi, D.L.; Lerner, D.L.; Fox, H.S.; Olmsted, R.A.; Bloom, F.E.; Henriksen, S.J.; Elder, J.H. Reading : Society for General Microbiology; 1994 May. The Journal of general virology v. 75 (pt.5): p. 979-987; 1994 May. Includes references. Language: English Descriptors: Cats; Feline immunodeficiency virus; Central nervous system; Cerebrospinal fluid; Brain; Lesions Abstract: Specific pathogen-free cats were infected with the Maryland strain of FIV (FIV-MD) for the purpose of assessing the effects of FIV infection on the central nervous system (CNS). Two separate studies were performed, involving a total of 13 infected cats and six age-matched, sham-inoculated controls. All animals infected with FIV-MD seroconverted by 8 weeks post-infection and virus was recovered from peripheral blood mononuclear cells of all infected cats. All of the infected animals had lower absolute CD4(+) cell counts and decreased CD4(+)/CD8(+) ratios. Virus was recovered from the cerebrospinal fluid (CSF) of certain infected individuals, and antiviral antibody and pleocytosis were evident in the CSF of the majority of infected cats. Additionally, virus was recovered from tissue explants from the cerebellum, midbrain and brainstem of one sacrificed FIV(+) cat. Specific neurological changes included anisocoria, delayed righting reflex and delayed pupillary reflex, as well as delayed visual and auditory evoked potentials, and marked alterations in sleep patterns similar to those reported for human immunodeficiency virus (HIV)-positive individuals. Histological evaluation revealed the presence of perivascular cuffing and glial nodules in FIV-infected cats. These results indicate that FIV causes an acute neurological disease that closely resembles the early neurological effects of HIV infection in humans and should serve well as an animal model for lentivirus-induced CNS disease. 237 NAL Call. No.: 410.9 P94 A new mouse strain manifesting high proteinuria and kinney glomerular defect. Hyun, B.H.; Wakasugi, N.; Nose, M.; Saito, T.; Tomita, T. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Oct. Laboratory animal science v. 41 (5): p. 442-446; 1991 Oct. Includes references. Language: English Descriptors: Mice; Mutants; Proteinuria; Glomerulopathy; Recessive genes; Animal models; Disease models Abstract: A mutant strain of mice manifesting high proteinuria, wasting syndrome, and kidney glomerular defect was established from the F5 offspring of an interstrain cross of CBA/Nga and RFM/Nga mice. Affected mice had high levels of proteinuria after 40 days of age. The body weight of about 22.6% of affected mice decreased rapidly and they died between 3 and 5 months of age. We learned that this abnormality is controlled by two pairs of autosomal recessive genes; the mutant strain of mice is designated FGS/Nga. The mutant strain has been characterized by high proteinuria and renal lesions with focal sclerosis of glomeruli and tubular atrophy with interstitial nephritis in the kidney resembling the human disease. The FGS/Nga mouse strain is a potential animal model for studying kidney glomerular defect in humans. 238 NAL Call. No.: 410.9 P94 A new rat mutant with chronic conjugated hyperbilirubinemia and renal glomerular lesions. Hosokawa, S.; Tagaya, O.; Mikami, T.; Nozaki, Y.; Kawaguchi, A.; Yamatsu, K.; Shamoto, M. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Feb. Laboratory animal science v. 42 (1): p. 27-34; 1992 Feb. Includes references. Language: English Descriptors: Rats; Mutants; Hyperbilirubinemia; Animal models; Hereditary diseases; Disease models; Glomerulus; Histopathology Abstract: A new mutant strain of inbred Sprague Dawley rats with autosomal recessive hyperbilirubinuria, were studied by biochemical, histologic, and ultrastructural methods. The plasma bilirubin concentration in the homozygote was significantly higher than that of the heterozygote, and about 80% of the bilirubin was conjugated. Plasma BSP and ICG clearance were both severely delayed in the homozygote. Plasma BSP elimination kinetics suggested that the pathophysiologic defect was not hepatic uptake or storage but rather in secretion into bile. Histopathology of the liver demonstrated brown pigment in the hepatocytes that appeared to be lipofuscin. The electron microscopic features of the hepatic pigment resembled those of the Dubin-Johnson syndrome. Homozygote histopathology also revealed glomerular lesions with mesangial expansion and proliferation in the kidneys. Immunohistologic studies disclosed mesangial granular deposition of IgG, IgA, and to a lesser degree, IgM and C3. These renal changes resembled those of IgA nephropathy. The spontaneous hyperbilirubinuric rat (EHBR) may be a useful animal model for studying constitutive conjugated hyperbilirubinemia, bilirubin metabolism, cholestasis, and glomerulonephropathy subsequent to hepatic dysfunction. 239 NAL Call. No.: RC262.C5N8 No effect of adult dietary fat on tumors induced prenatally by diethylstilbestrol. Walker, B.E. Hillsdale, N.J. : Lawrence Erlbaum Associates, Inc; 1992. Nutrition and cancer v. 17 (2): p. 161-169; 1992. Includes references. Language: English Descriptors: Female animals; Prenatal period; Diethylstilbestrol; Maturation; Dietary fat; Neoplasms Abstract: Strain CD-1 female mice exposed prenatally to diethylstilbestrol (DES) or vehicle were placed on semipurified diets containing 2.6%, 10%, 20%, or 29% fat by weight at four weeks of age. These mice were used as a breeding colony for a few weeks and then maintained to terminal illness on the semipurified diets. Females exposed prenatally to DES developed mammary tumors, pituitary tumors, and glandular tumors of the reproductive tract. There was no significant difference in tumor frequency between low- and high-fat dietary groups. Fewer tumors appeared in the vehicle- exposed mice, as expected, and their frequency did not differ between the dietary groups. Pregnancy reduced tumor frequency in DES-exposed mice, but the incidence of pregnancy was not significantly different between low- and high-fat dietary groups. In the adult the failure of a high-fat diet to increase the frequency of reproductive system tumors induced prenatally is in marked contrast to the effectiveness of high- fat diets in promoting mammary tumors induced by carcinogens given to rats postnatally. This difference is critical in the interpretation of epidemiological studies. The relationship of dietary fat to reproductive system cancer in human populations was reviewed in comparison with these two animal models. The epidemiological literature was found to be more consistent with the animal model, showing high sensitivity to dietary fat prenatally but no significant sensitivity at the adult stage of life. 240 NAL Call. No.: QL55.A1I43 The NOD mouse: a model for analyzing the interplay between heredity and environment in development of autoimmune disease. Leiter, E.H. Washington, D.C. : Institute of Laboratory Animal Resources, National Research Council; 1993. I.L.A.R. news v. 35 (1): p. 4-14; 1993. Includes references. Language: English Descriptors: Mice; Animal models; Autoimmune diseases 241 NAL Call. No.: QP141.H78 Nutrition and aging in animal models. Masoro, E.J. New York, N.Y. : Plenum; 1989. Human nutrition : a comprehensive treatise v. 6: p. 25-41; 1989. Includes references. Language: English Descriptors: Elderly nutrition; Laboratory animals; Food restriction; Caloric intake; Dietary proteins; Source fat; Nutrient intake; Minerals; Vitamins 242 NAL Call. No.: QP141.A1J685 Nutritional immunology: methodological considerations. Fraker, P. Binghamton, NY : Haworth Medical Press, c1991-; 1994. Journal of nutritional immunology v. 2 (4): p. 87-92; 1994. Paper presented at the Workshop on Nutrition, Immunity and Infection, October 7-9, 1992, Bethesda, Maryland. Includes references. Language: English Descriptors: Immunology; Nutritional state; Nutrition physiology; Immune response; Nutrient deficiencies; Animal models 243 NAL Call. No.: 500 N484 Nutritional influence on neonatal infections in animal models and man. Harris, M.C.; Douglas, S.D. New York, N.Y. : The Academy; 1990. Annals of the New York Academy of Sciences v. 587: p. 246-256; 1990. In the series analytic: Micronutrients and immune functions / edited by A. Bendich and Ranjit K. Chandra. Literature review. Includes references. Language: English Descriptors: Infant nutrition; Infectious diseases; Malnutrition; Neonates; Neutrophils; Rats; Animal models; Disease resistance; Literature reviews 244 NAL Call. No.: QH301.F3 Obesity, diabetes, and neoplasia in yellow A(vy)/-mice: ectipic expression of the agouti gene. Yen, T.T.; Gill, A.M.; Frigeri, L.G.; Barsh, G.S.; Wolfe, G.L. Bethesda, Md. : The Federation of American Societies for Experimental Biology; 1994 May. The FASEB journal : official publication of the Federation of American Societies for Experimental Biology v. 8 (8): p. 479-488; 1994 May. Includes references. Language: English Descriptors: Mice; Obesity; Diabetes; Mutations; Loci; Genes; Phenotypes; Metabolic disorders; Literature reviews; Animal models 245 NAL Call. No.: RC628.E97 1991 Obesity in Europe 91 proceedings of the 3rd European Congress on Obesity. Ailhaud, G. European Congress on Obesity 3rd : 1991 : Nice, France. London : John Libbey,; 1992. xii, 464 p. : ill. ; 25 cm. "Obesity in Europe 91 represents the edited proceedings of the 3rd European Congress on Obesity, held in Nice, France, 30 May-1 June 1991"--2nd prelim. page. Includes bibliographical references and indexes. Language: English Descriptors: Obesity Abstract: Discusses the multifaceted aspects of human obesity; neuro-endocrine regulation of food intake; the genetics of obesity in animal models and humans; epidemiological aspects of obesity; management of obesity; CNS-periphery relationships; enzymatic and metabolic regulation of adipose tissue; control of energy expenditure; cellular and molecular biology in the analysis of obesity; psychosocial aspects of obesity; etc. 246 NAL Call. No.: QP141.C65 Obesity--role of animal models. McCracken, K.J. London : J. Libbey; 1988. Comparative nutrition / editors, Sir Kenneth Blaxter, Ian Macdonald. p. 163-184; 1988. Literature review. Includes references. Language: English Descriptors: Obesity; Nutrition physiology; Animal experiments 247 NAL Call. No.: 389.8 J824 Omega-3 fatty acids in health and disease and in growth and development. Simopoulos, A.P. Baltimore, Md. : American Society for Clinical Nutrition; 1991 Sep. American journal of clinical nutrition v. 54 (3): p. 438-463. charts; 1991 Sep. Literature review. Includes references. Language: English Descriptors: Polyenoic fatty acids; Eicosapentaenoic acid; Docosenoic acids; Metabolism; Nutrient sources; Diet; Evolution; Food composition tables; Heart diseases; Hypertension; Inflammation; Autoimmune diseases; Neoplasms; Diabetes; Nutrient deficiencies; Disease prevention; Nutrition physiology; Literature reviews Abstract: Several sources of information suggest that man evolved on a diet with a ratio of omega 6 to omega 3 fatty acids of approximately 1 whereas today this ratio is approximately 10:1 to 20-25:1, indicating that Western diets are deficient in omega 3 fatty acids compared with the diet on which humans evolved and their genetic patterns were established. Omega-3 fatty acids increase bleeding time; decrease platelet aggregation, blood viscosity, and fibrinogen; and increase erythrocyte deformability, thus decreasing the tendency to thrombus formation. In no clinical trial, including coronary artery graft surgery, has there been any evidence of increased blood loss due to ingestion of omega 3 fatty acids. Many studies show that the effects of omega 3 fatty acids on serum lipids depend on the type of patient and whether the amount of saturated fatty acids in the diet is held constant. In patients with hyperlipidemia, omega 3 fatty acids decrease low-density-lipoprotein (LDL) cholesterol if the saturated fatty acid content is decreased, otherwise there is a slight increase, but at high doses (32 g) they lower LDL cholesterol; furthermore, they consistently lower serum triglycerides in normal subjects and in patients with hypertriglyceridemia whereas the effect on high-density lipoprotein (HDL) varies from no effect to slight increases. The discrepancies between animal and human studies most likely are due to differences between animal and human metabolism. In clinical trials eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA) in the form of fish oils along with antirheumatic drugs improve joint pain in patients with rheumatoid arthritis; have a beneficial effect in patients with ulcerative colitis; and in combination with drugs, improve the skin lesions, lower the hyperlipidemia from etretinates, and decrease the toxicity of cyclosporin in patients with psoriasis. In various animal models omega 3 fatty acids decrease the number and size of tumors and increase the time 248 NAL Call. No.: QL737.P6C6 v.25 Osteoarthritis in rhesus monkeys and gibbons a locomotor model of joint degeneration. DeRousseau, C. Jean Basel ; New York : Karger,; 1988. xii, 145 p. : ill. ; 25 cm. (Contributions to primatology ; v. 25). Includes index. Bibliography: p. [103]-131. Language: English Descriptors: Osteoarthritis; Animal models; Primates; Diseases; Medical anthropology 249 NAL Call. No.: SF380.I52 Ovine GM1 gangliosidosis. Murnane, R.D.; Ahern-Rindell, A.J.; Prieur, D.J. New York : Elsevier; 1991 Oct. Small ruminant research v. 6 (1/2): p. 109-115; 1991 Oct. Includes references. Language: English Descriptors: Sheep; Gangliosidosis; Lysosomes; Neurons; Histopathology; Diagnosis; Symptoms; Animal models 250 NAL Call. No.: 500 N484 Oxygen free radical-mediated heart injury in animal models and during bypass surgery in humans: effects of alpha-tocopherol. Ferrari, R.; Curello, S.; Boffa, G.M.; Condorelli, E.; Pasini, E.; Guarnieri, G.; Albertini, A. New York, N.Y. : The Academy; 1989. Annals of the New York Academy of Sciences v. 570: p. 237-253; 1989. In the series analytic: Vitamin E--biochemistry and health implications / edited by A.T. Diplock, L.J. Machlin, L. Packer and W.A. Pryor. Literature review. Includes references. Language: English Descriptors: Myocardial ischemia; Oxygen; Stress; Surgery; Vitamin e; Vitamin deficiency; Human nutrition research; Rats; Literature reviews 251 NAL Call. No.: 410.9 P94 Pancreatectomized swine as a model of diabetes mellitus. Stump, K.C.; Swindle, M.M.; Saudek, C.D.; Strandberg, J.D. Cordova, Tenn. : American Association for Laboratory Animal Science; 1988 Aug. Laboratory animal science v. 38 (4): p. 439-443. ill; 1988 Aug. Includes references. Language: English Descriptors: Pigs; Pancreatectomy; Disease models; Diabetes; Blood glucose; Insulin; Mortality Abstract: The development of a model of diabetes mellitus using swine offers the potential for new investigations in the study of human diabetic complications. In particular, animal models for the study of accelerated atherosclerosis associated with diabetes are important and presently lacking. Swine were selected because they have a natural susceptibility to atherosclerosis and have plasma lipoprotein patterns which are close to those of humans. Diabetes mellitus was induced in nine miniature swine by total pancreatectomy. Following surgery, they were maintained on porcine derived insulin at doses predicated on blood glucose levels. Pancreatic enzymes were replaced by dietary supplementation. Eight of the nine pigs were pancreatectomized successfully and stabilized with insulin. After initial weight loss, the pancreatectomized pigs maintained growth rates comparable to controls. Hypoglycemia and bacterial infections were the major problems experienced. Post-operative survival ranged from 50 days to 455 days. Our study shows that swine can be pancreatectomized successfully and maintained as insulin dependent animals, presenting a realistic model for research on the complications of diabetes. 252 NAL Call. No.: TX345.B74 The pathogenesis of obesity. Bray, G.A. San Diego, Calif. : Academic Press; 1989. Bristol-Myers Squibb/Mead Johnson nutrition symposia v. 7: p. 129-143. charts; 1989. In the series analytic: Nutrition and the Origins of Disease / edited by C.H. Halsted and R.B. Rucker. Literature review. Includes references. Language: English Descriptors: Obesity; Nutrient balance; Energy expenditure; Regulation; Feedback; Neurotransmitters; Brain; Sympathetic nervous system; Adrenalectomy; Nutrition physiology; Literature reviews Abstract: The regulation of body weight is presented as a controlled system for nutrient balance. Nutrient intake and storage; energy expenditure; a nutrient control equation; and animal models of obesity (hypothalamic, genetic and dietary) are discussed. The role of the brain (anatomy and neurotransmitters); feedback signals; and efferent controls as regulators of food intake and nutrient metabolism are also reviewed. 253 NAL Call. No.: DISS F1991140 Pathogenetische Rolle zytotoxischer T-Lymphozyten bei der Masernenzephalitis im Tiermodell [Pathogenetic relevance of cytotoxic T lymphocytes (CTL) in measles virus-induced encephalitis in two animal models]. Niewiesk, Stefan Hannover : [s.n.],; 1991. ix, 134 p. : ill. ; 21 cm. Summary in English. Includes bibliographical references (p. 107-126). Language: German 254 NAL Call. No.: QR1.I57 Pathogenicity of porcine intestinal spirochetes in gnotobiotic pigs. Neef, N.A.; Lysons, R.J.; Trott, D.J.; Hampson, D.J.; Jones, P.W.; Morgan, J.H. Washington, D.C., American Society for Microbiology; 1994 Jun. Infection and immunity v. 62 (6): p. 2395-2403; 1994 Jun. Includes references. Language: English Descriptors: Pigs; Spirochaetales; Pathogenicity; Phenotypes; Enzymes; Animal models; Colonization; Gnotobiotic animals; Bacteroids; Intestinal microorganisms; Yersinia pseudotuberculosis Abstract: Twelve intestinal spirochete strains of porcine origin were characterized on the basis of their phenotypic properties, by multilocus enzyme electrophoresis, and by pathogenicity testing in gnotobiotic pigs. The spirochetes used included two strains of Serpulina hyodysenteriae (B204 and P18A), two strains of Serpulina innocens (B256 and 4/71), one strain from the proposed new genus and species "Anguillina coli" (P34/6/78), and seven non-S. hyodysenteriae strains recently isolated from United Kingdom pigs herds with a history of nonspecific diarrhea and typhlocolitis. By multilocus enzyme electrophoresis, five of these were identified as S. innocens, one was identified as an unspecified Serpulina sp., and one was identified as "A. coli." S. hyodysenteriae B204 and P18A, "A. coli" P43/6/78 and 2/7, and three (22/7, P2801/1, and 14/5) of the five S. innocens field isolates induced mucoid feces and typhlocolitis in gnotobiotic pigs. None of the other spirochetes produced clinical signs or large intestinal pathology in this model. The "A. coli" strains induced a more watery diarrhea, with lesions present more proximally in the large intestine, than did the other pathogenic spirochetes. S. innocens 22/7 was also tested for pathogenicity in hysterotomy-derived pigs that had previously been artificially colonized with a spirochete- free intestinal flora and shown to be susceptible to swine dysentery. Despite effective colonization, strain 22/7 did not produce any disease, nor was there any exacerbation of large intestinal pathology or clinical signs when pigs with an experimentally induced existing colitis caused by Yersinia pseudotuberculosis were superinfected with strain 22/7. Certain non-S. hyodysenteriae spirochetes are therefore capable of inducing disease in gnotobiotic pigs, but their role as primary or opportunistic pathogens in conventional pigs remains equivocal. 255 NAL Call. No.: 410.9 P94 Pharmacokinetics of fusidic acid in laboratory animals. Findon, G.; Miller, T.E.; Rowe, L.C. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Oct. Laboratory animal science v. 41 (5): p. 462-465; 1991 Oct. Includes references. Language: English Descriptors: Rats; Mice; Rabbits; Guinea pigs; Antibiotics; Pharmacokinetics; Oral administration; Subcutaneous injection; Intramuscular injection Abstract: The ability to evaluate the efficacy of fusidic acid in animal models of infectious disease is limited by the absence of pharmacokinetic data for the agent in laboratory animals. In our study, aspects of fusidic acid pharmacokinetics were compared in rats (Rattus norwegicus), mice (Mus musculus), rabbits (Oryctolagus cuniculus), and guinea pigs (Cavia porcellus). Sodium fusidate was poorly absorbed after oral administration to rats, although limited absorption occurred in guinea pigs, mice, and rabbits. Subcutaneous injections of diethanolamine fusidate to laboratory rats, however, achieved a serum profile similar to that observed in humans. There was no evidence of drug accumulation in rats given repeated subcutaneous doses of diethanolamine fusidate during a 4-day period, but rabbits showed clear evidence of a cumulative effect. 256 NAL Call. No.: TD888.C65C68 1988 Physiologic and cellular changes in an animal model of byssinosis. Hara, K.S.; Scanlon, P.D.; Schroeder, M.A.; Rohrbach, M.S. Memphis, TN : National Cotton Council; 1988. Cotton dust : proceedings of the Twelfth Cotton Dust Research Conference, beltwide cotton research conferences, New Orleans, LA, January 6-7, 1988 / proc of Endotoxin Inhalation Workshop, Clearwater, FL, Sept 28-30, 1987. p. 171-175; 1988. Includes references. Language: English Descriptors: Guinea pigs; Cotton; Dusts; Respiratory diseases 257 NAL Call. No.: 389.1 W892 The piglet as a model animal for studying aspects of digestion and absorption in milk-fed human infants. Moughan, P.J.; Nirtles, M.J.; Cranwell, P.D.; Smith, W.C.; Pedraza, M. Basel : S. Karger; 1992. World review of nutrition and dietetics v. 67: p. 40-113; 1992. In the series analytic: Nutritional triggers for health and disease / edited by A. P. Simopoulos. Literature review. Includes references. Language: English Descriptors: Infants; Diet; Milk; Human milk; Digestion; Absorption; Animal models; Piglets; Literature reviews 258 NAL Call. No.: 41.8 Am3 Polysulfated glycosaminoglycan in the treatment of osteoarthritis. Todhunter, R.J.; Lust, G. Schaumburg, Ill. : The Association; 1994 Apr15. Journal of the American Veterinary Medical Association v. 204 (8): p. 1245-1251; 1994 Apr15. Includes references. Language: English Descriptors: Dogs; Horses; Glycosaminoglycans; Osteoarthritis; Drug therapy; Disease prevention; Drug effects; Enzymes; Inhibition; Animal models; Dosage; Adverse effects; Literature reviews 259 NAL Call. No.: 41.8 Ad9 Portosystemic hepatic encephalopathy related with congenital and acquired hepatopathies in the dog. Rothuizen, J. San Diego, Calif. : Academic Press; 1993. Advances in veterinary science and comparative medicine v. 37: p. 403-416; 1993. In the series analytic: Animal models in liver research / edited by Charles E. Cornelius. Includes references. Language: English Descriptors: Hepatitis; Cirrhosis; Portal vein; Hypoplasia; Encephalopathy; Animal models; Dogs; Vascular diseases; Literature reviews 260 NAL Call. No.: QP86.P6 The Potential for nutritional modulation of the aging process. Ingram, Donald K.; Baker, George T.; Shock, Nathan Wetherill, Trumbull, Conn. : Food & Nutrition Press,; 1991. xiii, 417 p. : ill. ; 24 cm. (Publications in food science and nutrition). Proceedings of an international conference sponsored by the American Health Foundation, co-sponsored by National Institutes on Aging, Food and Drug Administration, The Gerontological Society of America, September 13-15, 1988, New York, NY. Includes bibliographical references and index. Language: English Descriptors: Aging Abstract: Reports the proceedings of a conference on the fundamental effects of nutritional variables on aging processes. Variables range from population demography and epidemiology to biochemistry and molecular genetics to the involvement of nutritional variables in the etiology of specific diseases. Research on animal models of the effects of calorie restriction on a number of age-related phenomena ranging from genetic expression to learning and memory and the involvement of specific nutrients on age-related processes are presented. 261 NAL Call. No.: 500 N484 Prenatal protein malnutrition and postnatal brain function. Tonkiss, J.; Galler, J.; Morgane, P.J.; Bronzino, J.D.; Austin-Lafrance, R.J. New York, N.Y. : The Academy; 1993. Annals of the New York Academy of Sciences v. 678: p. 215-227; 1993. In the series analytic: Maternal nutrition and pregnancy outcome / edited by C.L. Keen, A. Bendich, and C.C. Willhite. Literature review. Includes references. Language: English Descriptors: Human nutrition research; Prenatal period; Protein deficiencies; Puerperium; Animal models; Brain; Neurophysiology; Literature reviews 262 NAL Call. No.: QR1.I57 Production and purification of heat-stable exterotoxin b from a porcine Escherichia coli strain. Dubreuil, J.D.; Faribrother, J.M.; Lallier, R.; Lariviere, S. Washington, D.C. : American Society for Microbiology; 1991 Jan. Infection and immunity v. 59 (1): p. 198-203; 1991 Jan. Includes references. Language: English Descriptors: Pigs; Rats; Escherichia coli; Enterotoxins; Heat stability; Purification; Characterization; Animal models Abstract: Production of heat-stable enterotoxin b (STb) by porcine Escherichia coli strains belonging to serogroup O115 was evaluated in ligated intestinal segments of adult rats. The conditions for optimal production and detection of STb were studied by using the STb-producing strain 4247. As STb production was similar in complex Trypticase soy broth and minimal Davis medium, the latter was used for the fermentation of strain 4247 and the production of STb in large quantities. STb was then purified to apparent homogeneity by sequential ultrafiltration, ultracentrifugation, and preparative gel electrophoresis. The enterotoxin was purified more than 500- fold and exhibited a molecular weight of approximately 5,000 as determined by urea-sodium dodecyl sulfate gel electrophoresis. Purified STb retained such chemical characteristics as resistance to heating (60 degrees C/30 min) and sensitivity to trypsin. A rabbit polyclonal antiserum was produced against the purified toxin. Numerous booster doses were required to obtain a significant enzyme-linked immunosorbent assay titer, suggesting that STb is a poor immunogen. Nevertheless, the antiserum was used successfully to discriminate between culture supernatants of STb-positive and STb-negative O115 E. coli strains, thus demonstrating the immunogenicity of purified STb. 263 NAL Call. No.: QP501.B474 A profile of cerebral and hepatic carnitine, ammonia, and energy metabolism in a model of organic aciduria:BALB/cByJ mouse with short-chain acyl-CoA dehydrogenase deficiency. Qureshi, I.A.; Ratnakumari, L.; Michalak, A.; Giguere, R.; Cyr, D.; Butterworth, R.F. Orlando, Fla. : Academic Press; 1993 Oct. Biochemical medicine and metabolic biology v. 50 (2): p. 145-158; 1993 Oct. Includes references. Language: English Descriptors: Metabolic disorders; Oxidoreductases; Enzyme deficiencies; Energy metabolism; Mice Abstract: Spontaneous animal models of inborn errors of metabolism are valuable tools for defining the pathogenesis of these disorders and also the mechanism of various therapeutic approaches. In the present study, we have employed BALB/cByJ mice with an autosomal recessive deficiency of short-chain acyl-CoA dehydrogenase (SCAD). These animals were characterized by a marked urinary excretion of ethylmalonic and methylsuccinic acids along with butyrylglycine. Using adult homozygous mice we have studied the basic cerebral and hepatic profile of carnitine, ammonia, and energy metabolism. The effects of fasting and a short-term supplement of L- carnitine have been evaluated in comparison with control BALB/cJ mice. The mutant mice had low levels of acetyl-CoA and high levels of lactate compared to control mice. Fasting aggravated this condition by further decreasing acetyl- CoA and increasing lactate levels in the mutant mice. Free carnitine levels were significantly decreased in liver with fasting. Long-chain acylcarnitines were significantly lower in the brain of mutant mice. A short-term supplementation of L- carnitine resulted in general increases of carnitine levels in liver and muscle, but they still remained lower in mutant BALB/cByJ mice as compared to control BALB/cJ mice. L- carnitine treatment increased cerebral CoA-SH levels and both hepatic and cerebral acetyl-CoA levels in mutant mice. Hyperammonemia which has been described frequently in acyl-CoA dehydrogenase deficiencies was not observed in adult BALB/cByJ mice. This could be due to a rapid conjugation of butyryl-CoA with glycine by an increased activity of glycine N- acyltransferase. 264 NAL Call. No.: QR1.I57 Protection of C3H/HeN mice from challenge with Borrelia burgdorferi through active immunization with OspA, OspB, or OspC, but not with OspD or the 83-kilodalton antigen. Probert, W.S.; LeFebvre, R.B. Washington, D.C., American Society for Microbiology; 1994 May. Infection and immunity v. 62 (5): p. 1920-1926; 1994 May. Includes references. Language: English Descriptors: Borrelia burgdorferi; Immunization; Mice; Surface antigens; Disease prevention; Antibody formation; Antibacterial properties Abstract: Recent advances in the development of animal models for Lyme borreliosis have provided means of identifying potential targets for the design of a subunit vaccine to prevent this disease. The C3R/HeN mouse model was used to study several Borrelia burgdorferi antigens from a single isolate for their ability to elicit borreliacidal and protective antibodies. The ospA, ospB, ospC, ospD, and 83-kDa genes from a California isolate, SON 188, were cloned and expressed in Escherichia coli as proteins fused to the C- terminal end of maltose-binding protein. Active immunization of mice with these fusion proteins elicited high titers of antibodies that recognized the homologous SON 188 antigens upon immunoblotting. Antibodies generated to the OspA and OspB fusion proteins, but not to the OspC, OspD, and the 83-kda fusion proteins, demonstrated in vitro borreliacidal activity. Challenge of all actively immunized mice with 10(7) SON 188 spirochetes resulted in infection in all mice receiving the OspD or 83-kDa immunogens but not in any mice receiving the OspA, OspB, or OspC fusion proteins. These results demonstrate the potential of OspA, OspB, and OspC as components of a subunit vaccine for the prevention of Lyme borreliosis. 265 NAL Call. No.: 410.9 P94 Pulmonary responses of conscious strain 13 guinea pigs to pichinde viral infection. Guo, Z.M.; Liu, C.T. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Dec. Laboratory animal science v. 41 (6): p. 581-584; 1991 Dec. Includes references. Language: English Descriptors: Guinea pigs; Pichinde virus; Animal models; Respiration; Measurement Abstract: A laboratory animal model for studying pulmonary responses to arenaviral infection was established with advanced technologies. Tidal volume (TV), respiratory rate (RR), minute volume (MV), expiratory time (TE), inspiratory time (TI), peak expiratory flow (PEF), and specific pulmonary airway resistance (RES) were measured with a double plethysmograph and a computer data-acquisition system in six conscious, strain 13 guinea pigs. Using the same animal, experiments were conducted before and after subcutaneous inoculation with 10(4) plaque-forming units of Pichinde virus. Pulmonary functions were determined for 1 minute every 10 minutes for 2 hours before and at postinoculation days (PUD) 3, 6, 8, and daily thereafter until shortly before death. The mean time to death was 18 +/- 0.7 days. Tidal volume, RR, MV, PEF, RES, and rectal temperature increased slightly on PID 3 and reached peak values at the midpoint of disease. At 95% of the mean time to death (16.5 +/- 0.5 days), RR, MV, and rectal temperatures suddenly decreased to lower than baseline values; while TV, RES, and PEF values remained high. When TE decreased with the increase in RR, TI did not change. When RR decreased at the terminal stage, both TE and TI increased. Hyperventilation, increased specific pulmonary airway resistance, terminal hypoventilation, and respiratory arrest were noted in strain 13 guinea pigs infected with Pichinde virus. 266 NAL Call. No.: RA1190.F8 Quantitative analysis of neuronal damage induced by tri-ortho- cresyl phosphate in Wistar rats. Inui, K.; Mitsumori, K.; Harada, T.; Maita, K. Orlando, Fla. : Academic Press; 1993 Jan. Fundamental and applied toxicology : official journal of the Society of Toxicology v. 20 (1): p. 111-119; 1993 Jan. Includes references. Language: English Descriptors: Organophosphorus compounds; Toxicity; Neurotoxins; Nervous system diseases; Neurons; Histopathology; Ultrastructure; Animal models; Toxicology; Rats Abstract: A quantitative analysis of neuronal damage was performed on the fasciculus gracilis (FG) of the cervical spinal cord in male Wistar rats that received orally a single dose of tri-ortho-cresyl phosphate (TOCP) at 1500 mg/kg. FG tissues were sampled at 1, 2, and 3 weeks after treatment and examined histopathologically. Wallerian degeneration of myelinated nerve fibers was observed in FG at 2 weeks. Morphological changes were most evident at 3 weeks after treatment and the number of fibers was reduced. Ultrastructurally, axonal swelling due to the accumulation of cytoplasmic contents was observed near the node of Ranvier in the affected animals, indicating paranodal degeneration. Axonal atrophy and swelling in organophosphorus-induced delayed neuropathy (OPIDN) were evaluated quantitatively using a computer-assisted image analyzer. Morphometric examinations on semi-thin sections and frozen sections stained with Nauta's method were demonstrated to be useful for objective evaluation of OPIDN in the rat. 267 NAL Call. No.: 41.9 AM37 Quantitative TC-99m-MDP joint scintigraphy in a lentivirus- induced arthritis of goats. Papageorges, M.; Gavin, P.R.; Barbee, D.D.; Sande, R.D.; Knowles, D.P.; Cheevers, W.P. Raleigh, N.C. : American College of Veterinary Radiology; 1991 Mar. Veterinary radiology v. 32 (2): p. 82-86; 1991 Mar. Includes references. Language: English Descriptors: Goats; Scintigraphy; Technetium; Caprine arthritis encephalitis virus; Arthritis; Inflammation; Joints (animal); Histopathology; Animal models 268 NAL Call. No.: RC262.C5N8 A rationale for dietary intervention in postmenopausal breast cancer patients: an update. Cohen, L.A.; Rose, D.P.; Wynder, E.L. Hillsdale, N.J. : Lawrence Erlbaum Associates, Inc; 1993. Nutrition and cancer v. 19 (1): p. 1-10; 1993. Literature review. Includes references. Language: English Descriptors: Mammary gland neoplasms; Nutritional intervention; Dietary fat; Nutrient intake; Risk; Women; Epidemiological surveys; Animal models; Feasibility studies; Literature reviews Abstract: In 1982, we proposed a large-scale randomized prospective trial to test the hypothesis that decreasing dietary fat intake from 38% to 20% of total calories would increase the disease-free interval and/or five-year survival rate for postmenopausal breast cancer patients. We now review new evidence from epidemiological studies, laboratory animal model studies, and preliminary feasibility trials that has accumulated over the past decade, in support of such a trial, and suggest that a more appropriate dietary goal is a reduction in fat intake to 15% of total calories. 269 NAL Call. No.: 442.9 SO1 Reduced survival of neonates due to vitamin A deficiency during pregnancy in the guinea pig. Apgar, J.; Dulin, A.; Kramer, T.; Smith, J.C. Baltimore, Md. : Williams & Wilkins; 1991 May. Proceedings of the Society for Experimental Biology and Medicine v. 197 (1): p. 56-58; 1991 May. Includes references. Language: English Descriptors: Vitamin a deficiency; Pregnancy; Survival; Newborn animals; Guinea pigs; Animal models; Mineral nutrition Abstract: Neonatal vitamin A stores are limited even in well- nourished full-term infants and are yet smaller in the premature infant. The object of this experiment was to determine whether vitamin A deficiency could be induced inpregnant guinea pigs and, if so, whether it would affect vitamin A status of the neonate.Adult (600 g) guinea pigs were fed a casein-agar diet that was vitamin A deficient (AD).Controls (vitamin A adequate) were orally dosed weekly with 2 mg of retinylpalmitate. Weight gains of dams and birth weights of neonates did not differ. No externalsigns of deficiency were observed. Six of eight AD and seven of eight vitamin A-adequatedams carried pregnancy to term (greater than or equal to Day 64). One AD dam died during delivery. Liver retinol concentrations were below the detection limit (<3 microgram/g) for all AD neonatesand dams and in postpartum serum of AD dams. Of neonates born greater than or equal to Day64, 15 of 18 AD were dead or moribund compared with 4 of 22 vitamin A adequate. The unexpectedly severeeffect on the neonate indicates that the guinea pig will be a sensitive modelfor investigating the affect of poor maternal vitamin A status on neonatal vitaminA-dependent functions. However, a less severe maternal deprivation should be used forsuch studies. 270 NAL Call. No.: 381 B522 Reduction of hyperlipidemia in the LA/N-corpulent rat by dietary fish oil containing n-3 fatty acids. Dolphin, P.J.; Amy, R.M.; Koeslag, D.G.; Limoges, B.F.; Russell, J.C. Amsterdam : Elsevier Science Publishers; 1988 Oct14. Biochimica et biophysica acta : International journal of biochemistry and biophysics v. 962 (3): p. 317-329; 1988 Oct14. Includes references. Language: English Descriptors: Rats; Obesity; Diet; Fish oils; Fatty acids; Hypertriglyceridemia Abstract: The LA/N rat, when homozygous for the corpulent gene (cp/cp), is obese, hyperphageous, hyperinsulinemic, hypertriglyceridemic and prone to the development of vascular and myocardial lesions. The hypertriglyceridemia, which in 3- month-old cp/cp males is 282 +/- 42 mg/dl and in females, 512 +/-83 mg/dl, results from the presence of a large triacylglycerol-rich VLDL. The moderate hypercholesterolemia in these animals is largely due to markedly elevated HDL levels, which reach 172 +/- 21 mg total lipid/dl in males and 154 +/- 22 mg total lipid/dl in females. The LA/N-cp rat is thus an interesting animal model of endogenous hypertriglyceridemia in which to examine the hypolipidemic effects of pharmacological agents and also dietary oil supplements containing the n-3 fatty acids. In this study, 1- month-old male and female cp/cp rats were fed a normal low fat laboratory chow supplemented with either 10% olive oil or 10% redfish (Sebastes marinus) oil ad libitum for a period of 2 months. The redfish oil contained 4.9 +/- 0.1% of its total fatty acids as eicosapentaenoic (20:5(n-3)) and 2.3 +/- 0.5% as docosahexaenoic acid (22:6(n-3)), the predominant fatty acids being gondoic (20:1(n-3)), 21.9 +/- 0.9% and cetoleic acid (22:1(n-11)), 21.7 +/- 1.7%, which are of dietary origin. Daily caloric was similar in the oil-fed versus control rats. However, the oil-fed animals weighed significantly more than the controls after 2 months of oil supplementation. Redfish oil reduced serum triacylglycerols by 54% in males and 45% in females after 2 months. VLDL levels, after the same time period, were reduced by 44% in males and 39% in females. HDL lipid mass was significantly reduced in both sexes (by 27% in males and 49% in females). However, the levels remained above those of male LA/N +/+ rats of the same age and Long-Evens rats. Olive oil feeding significantly reduced serum cholesterol, triacylglycerols and phospholipids in male but only cholesterol and phospholipids in female anim 271 NAL Call. No.: 381 J8282 Reevaluation and application of the dual-isoptope plasma ratio method for the measurement of intestinal cholesterol absorption in the hamster. Turley, S.D.; Herndon, M.W.; Dietschy, J.M. Bethesda, Md. : Lipid Research, inc., 1959-; 1994 Feb. Journal of lipid research v. 35 (2): p. 328-339; 1994 Feb. Includes references. Language: English Descriptors: Cholesterol; Intestinal absorption; Measurement; Isotope labeling; Blood plasma; Ratios; Biological techniques; Hamsters Abstract: These experiments systematically evaluated the dual-isotope plasma ratio method for measuring intestinal cholesterol absorption in the hamster. It was found that while the ratio of the and 14C-labeled cholesterol in the plasma, relative to the respective dose of each that was given, became constant by 72 h after their administration, the percent cholesterol absorption was lower in animals that were fasted before dosing (35.7 +/- 5.5%) than in their fed controls (47.5 +/- 3.7%). Furthermore, the percent absorption found 72 h after dosing varied greatly, depending on whether the intragastric dose of labeled cholesterol was administered in medium chain triglyceride (MCT) oil (46.2 +/- 2.3%), olive oil (63.9 +/- 11.2%), or safflower oil (74.6 +/- 4.5%). The level of absorption was not different between hamsters that had unrestricted (46.3 +/- 1.6%) and restricted (43.8 +/- 2.2%) access to their stools during the 72 h after dosing. Other experiments, using only hamsters in the fed state and MCT oil as the intragastric dosing medium, showed that the percent cholesterol absorption could be made to vary over a wide range using treatments known to produce such effects in humans. Thus, feeding either surfomer, cholestyramine, ursodeoxycholic acid, or CI-976, a new inhibitor of acyl-CoA:cholesterol acyltransferase, significantly blocked cholesterol absorption, whereas the addition of either cholic acid or increasing amounts of oil to the diet had the opposite effect. The modified dual-isotope plasma ratio method described here provides a simpler and more physiologic approach to the routine measurement of cholesterol absorption in the hamster and similar small animal models. 272 NAL Call. No.: 44.8 J822 Relationship of in vitro immune function with health and production in Holstein cattle. Weigel, K.A.; Freeman, A.E.; Kehrli, M.E. Jr; Thurston, J.R.; Kelley, D.H. Champaign, Ill. : American Dairy Science Association; 1992 Jun. Journal of dairy science v. 75 (6): p. 1672-1679; 1992 Jun. Includes references. Language: English Descriptors: Dairy cows; Immune competence; Animal health; In vitro; Assays; Bovine mastitis; Costs; Regression analysis; Milk production; Disease resistance; Screening Abstract: Eighty-seven lactating Holstein cows from the Iowa State University Breeding Research Herd were evaluated for 20 in vitro measures of immune function. Principal component analysis was used to discard redundant assay variables such that the 11 remaining variables were more nearly independent than the original variables. Multiple linear regression in an animal model was used to determine the effects of these 11 variables on lifetime production and on general udder, and reproductive health traits. A significant joint effect of the 11 immune function variables on California mastitis test scores was observed. California mastitis test scores were positively correlated with antibody-dependent neutrophil cytotoxicity and negatively correlated with antibody- independent neutrophil cytotoxicity. Wisconsin mastitis test scores were also positively associated with antibody-dependent neutrophil cytotoxicity. Cytochrome c reduction was negatively associated with mammary and total health costs. A positive relationship between clinical mastitis and discarded milk and IgG2 was observed, and IgG1 was associated with increased quarter California mastitis test scores and increased production. Thus, certain in vitro immune function assays may serve as indicators of susceptibility to health problems in dairy cattle, particularly for traits associated with udder health. 273 NAL Call. No.: 410.9 P94 A reproducible method for producing and quantifying the stages of fracture repair. Bourque, W.T.; Gross, M.; Hall, B.K. Cordova, Tenn. : American Association for Laboratory Animal Science; 1992 Aug. Laboratory animal science v. 42 (4): p. 369-374; 1992 Aug. Includes references. Language: English Descriptors: Mice; Bone fractures; Healing Abstract: Male CD-1 mice, 4 to 6 months of age, were used to establish a reproducible model to study the stages of fracture repair. A custom-designed fracture apparatus was constructed, and trials with it demonstrated its capacity to reliably reproduce a closed fracture of the tibia. Dietary and sleep habits in the treated mice were the same as unfractured control mice. Four stages of fracture repair were documented and the duration of each stage was quantifiable and reproducible. The last stage of fracture repair was completed by 21 days postfracture. The reproducibility of the fracture, the reproducibility of the times and stages of fracture repair, the relatively short time to complete the fracture repair process, and the minimal discomfort which allowed the mice to maintain a normal daily routine, suggest that this is an ideal animal model for studying the fracture repair process. 274 NAL Call. No.: Z6658.R47 Research utilization of miniature swine. Wilmington, Mass.? : Charles River, [between 1988-1990?]; 1988-1990. 83 p. ; 28 cm. Cover title. Language: English Descriptors: Diseases; Animal models; Bibliography; Swine as laboratory animals; Bibliography; Swine; Physiology; Bibliography 275 NAL Call. No.: QR1.I57 Restricted ability of group B streptococcal C5a-ase to inactivate C5a prepared from different animal species. Bohnsack, J.F.; Chang, J.K.; Hill, H.R. Washington, D.C. : American Society for Microbiology; 1993 Apr. Infection and immunity v. 61 (4): p. 1421-1426; 1993 Apr. Includes references. Language: English Descriptors: Streptococcus; Attractants; Inactivation; Strain differences Abstract: Most strains of group B streptococci (GBS) elaborate a cell surface-associated enzyme that rapidly inactivates the human complement-derived chemoattractants C5a and C5a(desarg) by cleaving the His-Lys bond at positions 67 and 68 in the C5a molecule. We have suggested that rapid inactivation of C5a and C5a(desarg) by this enzyme, called C5a-ase, can hinder the inflammatory response at sites of GBS infection. We tested the ability of GBS C5a-ase to inactivate C5a preparations from various animal species to determine the proper species for studying the role of GBS C5a-ase in the pathogenesis of GBS infections. Exposure of C5a preparations from humans, monkeys, and cows to GBS caused inhibition of C5a functional activity as measured by the ability of C5a to stimulate human polymorphonuclear leukocyte (PMN) adherence and human PMN chemotaxis. Bovine PMN chemotaxis to bovine C5a was also abolished after exposure of bovine C5a to GBS. In contrast, mouse, rat, guinea pig, rabbit, pig, and sheep C5a preparations retained full functional activity after exposure to GBS as measured by chemotaxis of human PMNs, PMNs from the same animal species, or both. These data suggest that there are structural differences between C5a proteins from different species which alter their susceptibility to GBS C5a-ase and indicate that most commonly used animal models of human GBS infection are inadequate for detection of a contribution of GBS C5a-ase to GBS virulence. 276 NAL Call. No.: RA421.P684 Retinoids or carotenoids: is there another choice?. Greenberg, E.R. Orlando, Fla. : Academic Press; 1993 Sep. Preventive medicine v. 22 (5): p. 723-727; 1993 Sep. Paper presented at the Fourth International Conference on Prevention of Human Cancer: Nutrition and Chemoprevention Controversies, June 3-6, 1992, Tucson, Arizona. Includes references. Language: English Descriptors: Retinoids; Carotenoids; Carcinoma; Disease prevention; Toxicity; Epidemiological surveys; Diet; Clinical trials; Antioxidants; Vitamin supplements; Literature reviews Abstract: Both retinoids and carotenoids decrease cancer occurrence in selected animal models of carcinogenesis, but the retinoids appear to have more potent activity against a wider variety of tumors. Future use of retinoids for cancer prevention will be limited, however, because of their toxic effects on bone and skin (among other organs). In contrast to retinoids, carotenoids seem to be free of important toxicity and this fact makes them more promising for use in the general adult population. However, the idea that carotenoids have a cancer-preventive effect in humans is based almost entirely on epidemiological studies of diet and serum which could simply reflect the effects of some other dietary constituents. In the search to explain the profoundly lower risk of death associated with eating a diet high in fruits, vegetables, and grains, there is a place for clinical trials testing one specific nutrient, such as beta-carotene, against one disease, such as lung cancer, but we should not rely exclusively on these narrowly focused studies. In addition, careful analyses of cohort studies may reveal broad patterns of diet that are associated with lower mortality. These diets can then be tested in clinical trials for their efficacy against a variety of causes of death and disability. For now, the most rational and prudent choice would be to consume a diet high in fruits, vegetables, and grains and not to take either supplemental antioxidants or retinoids until there is clear evidence of their effectiveness and safety. 277 NAL Call. No.: RC628.N48 1987 Reversible impairment of glucose-induced insulin secretion in SHR/N-cp rats. Voyles, N.R.; Powell, A.M.; Timmers, K.I.; Wilkins, S.D.; Bhathena, S.J.; Hansen, C.; Michaelis, O.E. IV; Recant, L. Bethesda, Md. : National Institutes of Health; 1988. New models of genetically obese rats for studies in diabetes, heart disease, and complications of obesity : NIH workshop, June 18-19, 1987, summaries of workshop papers and current bibliography. p. 33-44; 1988. Includes references. Language: English Descriptors: Animal models; Obesity; Diabetes; Rats 278 NAL Call. No.: 389.8 AM34 Review of clinical studies on cholesterol-lowering response to soy protein. Carroll, K.K. Chicago, Ill. : The Association; 1991 Jul. Journal of the American Dietetic Association v. 91 (7): p. 820-827; 1991 Jul. Literature review. Includes references. Language: English Descriptors: Soy protein; Hypercholesterolemia; Triacylglycerols; Low density lipoprotein; Animal experiments; Man; Literature reviews; Cholesterol; Blood serum; Blood plasma; Dietary protein Abstract: Experiments on animals have shown that soybean protein has hypocholesterolemic and antiatherogenic properties. In human beings, substitution of soy protein for dietary animal protein or addition of soy protein to the diet lowers total and low-density-lipoprotein cholesterol levels in individuals with hypercholesterolemia. Reductions of 20% or more have been obtained with diets high in protein (about 20% of total energy) and relatively low in fat. Triglycerides are also decreased, particularly in subjects with hypertriglyceridemia, but soy-protein diets appear to have little effect on high-density-lipoprotein cholesterol levels. Responses are similar in men and women, but may be greater in younger than in older subjects. The hypocholesterolemic effect is thought to be mainly attributable to the protein itself rather than to nonprotein components of soy-protein preparations. The mechanism of action is not known, and it may not be possible to explain the observed effects in human beings and in experimental animal models by the same mechanism. Although the hypocholesterolemic response to dietary soy protein has been observed by a number of European research groups, substitution of soy protein for animal protein in North American diets has generally had little effect, for reasons that are still not clear. 279 NAL Call. No.: 389.8 J82 A review of experimental studies of iodine deficiency during fetal development. Hetzel, B.S.; Mano, M.T. Bethesda, Md. : American Institute of Nutrition; 1989 Feb. The Journal of nutrition v. 119 (2): p. 145-151; 1989 Feb. Literature review. Includes references. Language: English Descriptors: Maternal nutrition; Mineral deficiencies; Iodine; Hypothyroidism; Goiter; Cretinism; Fetus Abstract: Iodine deficiency is now recognized as a major international public health problem. It is estimated that 800 million people may be at risk of the effects of iodine deficiency. In humans, the effects occur at all stages of development: the fetus, the neonate, the child and adult. The effects are now denoted by the term iodine deficiency disorders (IDD). They include miscarriages, stillbirths, congenital anomalies, as well as the more familiar goiter, cretinism, impaired brain function, and hypothyroidism in children and adults. In domestic animals, reproductive failure has been reported with the production of aborted, stillborn and weak calves. Experimental studies in animal models have been reviewed to provide evidence of the mechanisms involved, particularly in relation to brain development. The findings in three different species (rat, sheep, monkey) indicate that the effects are mediated by a combination of maternal and fetal hypothyroidism, the effect of maternal hypothyroidism being earlier than the onset of fetal thyroid secretion. The findings suggest that iodine deficiency has an early effect on neuroblast multiplication and, if so, this could be important in the pathogenesis of the neurological form of endemic cretinism. The assessment of the full effects of iodine deficiency on the brain requires further studies in the postnatal period to determine the duration of these effects. 280 NAL Call. No.: 410.9 P94 The role of Branhamella catarrhalis in the "bloody-nose syndrome" of cynomolgus macaques. VandeWoude, S.J.; Luzarraga, M.B. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Oct. Laboratory animal science v. 41 (5): p. 401-406; 1991 Oct. Includes references. Language: English Descriptors: Macaca fascicularis; Branhamella; Respiratory diseases; Nose; Hemorrhage; Pathogens Abstract: During a 15-month period, 25 cynomolgus macaques (Macaca fascicularis) at the Johns Hopkins University were observed to have nasal discharge. Fifteen (60%) of these animals had positive nasal cultures for Branhamella catarrhalis. Clinical signs associated with infection by this bacterium were sneezing, epistaxis, and mucohemorrhagic nasal discharge. Treatment with antibiotics resulted in prompt resolution of clinical signs. Post-therapeutic nasal cultures were negative for B. catarrhalis. Two groups of clinically normal, culture-negative, cynomolgus macaques were inoculated with natural isolates of B. catarrhalis which had been passaged in culture for various amounts of time. Five of the eight animals inoculated became culture-positive and had mild nasal discharge. Presence of blood on nasal swabs was indicative of infection with B. catarrhalis. Three of the inoculated animals had post-swabbing epistaxis. This report documents the role of B. catarrhalis as an upper respiratory pathogen in the cynomolgus monkey which causes mild self- limiting disease reminiscent of the so-called "Bloody-Nose Syndrome." In addition to the obvious clinical significance of this finding to primate clinicians, development of an animal model for human disease caused by this organism may be possible. 281 NAL Call. No.: QP141.A1N88 Role of omega-3 fatty acids in health and disease. Fernandes, G.; Venkatraman, J.T. Tarrytown, N.Y. : Pergamon Press; 1993. Nutrition research v. 13 (suppl.1): p. S19-S45; 1993. Paper presented at the 5th International Meeting on Advances in Infantile Nutrition, November 12-14, 1992, Naples, Italy. Includes references. Language: English Descriptors: Polyenoic fatty acids; Dietary fat; Diet; Fish oils; Fat consumption; Trends; Monoenoic fatty acids; Nutrition physiology; Infant development; Elderly; Fat deficiencies; Cardiovascular diseases; Carcinoma; Autoimmune diseases; Immune response; Rheumatoid arthritis; Nutritional intervention; Supplements; Enteral feeding; Parenteral feeding; Drug toxicity; Literature reviews Abstract: Dietary lipid interventions have an important role in modulating the onset of autoimmunity, cardiovascular diseases and cancer. Many studies carried out in the past have established the adverse effects of saturated fats in humans and in animal models. Based on these adverse effects, the consumption of vegetable oils containing both monounsaturated omega-9 and polyunsaturated fatty acids (rich in 18:2 omega-6) is rising significantly in the United States. The increased consumption of many vegetable oils particularly of omega-6 series is however to be viewed as pro-inflammatory and is suspected as one of the possible causes for the gradual rise in certain malignant tumors, rheumatoid arthritis and autoimmune diseases primarily due to the increased production of pro-inflammatory cytokines although its increased usage has reduced cardiovascular disease nearly 30% in the United States. Diets based on omega-6 enriched oils can increase the level of linoleic acid in tissue phosphoglycerides and are able to reduce cholesterol levels, yet these lipids usually tend to elevate excessive arachidonic acid (20:4 omega-6) levels. In contrast, omega-3 fatty acid-enriched fish oil (FO) and/or omega-3 precursors from certain vegetable oils (linolenic acid, 18:3 omega-3) are found to provide protection against cardiovascular disease, rheumatoid arthritis, cancer and possibly against the severity of viral infections. Nutritional modification of cellular functions by dietary lipids with a balanced ratio of omega-6 and omega-3 fatty acids offers an attractive avenue to correct, modify and/or prevent many patho-physiological processes in health and disease state and to reduce toxicity of drugs in many patients. The mediation of such effects is thought to be primarily achieved through alterations of cellular membranes composition and other endogenous lipid stores which may modify the functional activity of various receptors on plasma membranes. In summary, the protective effects of omega-3 lipids have been explained based on changes in eicosanoid synthesis and the reduced risk of sudden death from cardiac arrthyhmia, increased protection from ischemic myocardium, improved myocardial function and reduction of other cardiovascular and autoimmune disease risks. However, well- designed studies are still required to further define vegetable sources, both as a supplement to infant nutrition specifically for optimizing the development of cognitive function, and also as preventive measure for reducing the incidence of diseases of aging in rapidly growing elderly populations. 282 NAL Call. No.: 389.8 J82 The role of the cytokines, interferon alpha and tumor necrosis factor in the hypertriglyceridemia and wasting of AIDS. Grunfeld, C.; Feingold, K.R. Bethesda, Md. : American Institute of Nutrition; 1992 Mar. The Journal of nutrition v. 122 (3S): p. 749-753; 1992 Mar. Proceedings of a symposium on "Nutrition, Immunomodulation and AIDS" held at the American Institute of Nutrition Annual Meeting, April 21-25, Atlanta, GA. Literature review. Includes references. Language: English Descriptors: Acquired immune deficiency syndrome; Hypertriglyceridemia; Infections; Cachexia; Lipid metabolism; Immunological factors; Blood lipids; Interferon; Interleukins; Literature reviews Abstract: The hypertriglyceridemia of infection is mediated by many of the cytokines that regulate the immune response, including the tumor necrosis factors, the interleukins and the interferons. In the acquired immunodeficiency syndrome (AIDS), hypertriglyceridemia is most likely due to increased circulating levels of interferon alpha. Both in AIDS and in animal models there is no direct association between the presence of hypertriglyceridemia and the syndrome of wasting. Rather, circulating lipoproteins may neutralize infectious organisms and therefore contribute to host defense. 283 NAL Call. No.: QD415.A1B52 Saturated fatty acid, but not cholesterol, regulates apolipoprotein AI gene expression by posttranscriptional mechanism. Srivastava, R.A.K. Marrickville, N.S.W., Australia : Academic Press; 1994 Sep. Biochemistry and molecular biology international v. 34 (2): p. 393-402; 1994 Sep. Includes references. Language: English Descriptors: Dietary fat; Cholesterol; Saturated fats; Apolipoproteins; Gene expression; Genetic regulation; High density lipoprotein Abstract: The aim of the present study was to investigate the regulation of the apoAI gene by dietary saturated fat and cholesterol Saturated fatty acids and cholesterol raise low density- and high density lipoprotein particles in humans Increased LDL is attributed to the down-regulation of LDL- receptor gene, but the mechanism of increased plasma HDL levels is unknown To study the mechanism of HDL elevation by saturated fat, male rats and male mice were employed as animal models. since they also raise their plasma HDL levels when fed high lipid diets Animals were divided in four groups and fed the following diets: control (5% corn oil); high cholesterol (05%): high fat (20% coconut oil). and high fat plus cholesterol diets The high cholesterol diet did not alter plasma and HDL-cholesterol levels However, the high fat diet increased HDL levels by 20% in rats and 55% in mice. A combination of saturated fat and cholesterol diet raised plasma HDL levels by 36 and 67% in rats and mice respectively. Plasma apoAI levels increased parallel to HDL concentrations. Mechanism of HDL elevation by saturated fat was investigated Hepatic and intestinal apoAI mRNA did not change with any of the test diets in mice. Rat hepatic apoAI mRNA was also unchanged by the high cholesterol diet, but was decreased on high fat and fat-cholesterol combination diets These results suggest that transcriptional regulation of the apoAI gene was not responsible for increased plasma apoAI and HDL The translational efficiency of apoAI on isolated polysomes was also measured, and it was found that apoAI synthesis increased about 20% on high fat and fat-cholesterol combination diets This partially explains the elevated levels of plasma HDL. Additional regulation through impaired catabolism of HDL particles by high fat diet feeding may be another pathway for increased HDL levels Unlike apoAI mRNA, the mRNA of other HDL apoproteins, apoAII and apoAIV, were increased by high fat and combination diet feeding These results suggest that saturated fatty acids regulate plasma HDL levels by translational and posttranslational mechanisms. 284 NAL Call. No.: QH527.J68 Seasonal affective disorders: animal models non fingo. Zucker, I. New York, N.Y. : Guilford Publications; 1988. Journal of biological rhythms v. 3 (2): p. 209-223. ill; 1988. Includes references. Language: English Descriptors: Laboratory animals; Animal behavior; Seasonal behavior; Research 285 NAL Call. No.: 442.9 SO1 Selenium and sulfur in antioxidant protective systems: relationships with vitamin E and malaria. Levander, O.A. Baltimore, Md. : Williams & Wilkins; 1992 Jun. Proceedings of the Society for Experimental Biology and Medicine v. 200 (2): p. 255-259; 1992 Jun. Proceedings of a "Conference on Molecular and Comparative Nutrition," July 22-24, 1991, National Institutes of Health, Bethesda, Maryland. Includes references. Language: English Descriptors: Selenium; Sulfur; Vitamin e; Antioxidants; Glutathione peroxidase; Hydrolases; Proteins; Fish oils; Qinghaosu; Nutrient deficiencies; Malaria; Mice; Animal models Abstract: The metabolic relationships among the antioxidant nutrients selenium, sulfur, and vitamin E are particularly close. Selenium and vitamin E have long been known to spare one another in certain nutritional diseases of animals, and selenium has been considered to have a key antioxidant defense function as a component of glutathione peroxidase. However, the antioxidant role of glutathione peroxidase has been questioned and now proteins containing selenium have been identified: phospholipid hydroperoxide glutathione peroxidase, selenoprotein P, and iodothyronine deiodinase. Glutathione peroxidase activity independent of selenium resides in the glutathione S-transferases. Glutathione participates in both enzymatic and nonenzymatic antioxidant defense systems. Some low-molecular weight selenium compounds (e.g., ebselen) exhibit glutathione peroxidase-like action. Certain low molecular weight thiols decompose peroxides nonenzymatically (e.g., the ovothiols). Murine malaria appears to be a useful experimental model for investigating interrelationships of selenium and vitamin E. Vitamin E deficiency protects against the parasite, especially when the mice are concurrently fed peroxidizable fat such as fish or linseed oils. Selenium deficiency, on the other hand, has little or no protective effect against the parasite. Any practical utility of pro- oxidant diets in combating human malaria remains to be determined. 286 NAL Call. No.: 389.8 J82 Serum lipoprotein profiles in mice: effects of early over- and undernutrition. Aubert, R.; Camus, M.C.; Bourgeois, F.; Herzog, J.; Lemonnier, D. Bethesda, Md. : American Institute of Nutrition; 1988 Oct. The Journal of nutrition v. 118 (10): p. 1190-1196; 1988 Oct. Includes references. Language: English Descriptors: Overfeeding; Undernutrition; Litter size; Blood serum; Lipoproteins; Neonates; Mice Abstract: Effects of early over- and undernutrition on lipoprotein profiles of adult Swiss male mice reared in litters of different sizes were investigated. Lipoproteins were isolated by density gradient ultracentrifugation and defined by chemical composition. Protein moieties were defined by their charges. The lipoprotein lipase (LPL) activity in epididymal adipose tissue, heart and diaphragm was measured. Early feeding patterns induced permanent body weight differences in adult mice. Serum phospholipid content was significantly higher in obese than in control mice. Overfeeding led to significantly higher activity of LPL in adipose tissue; inversely, undernutrition induced a lower LPL activity. There was a trend toward variations of lipoprotein concentrations in relation to litter size, with significant differences being observed only between obese and undernourished mice for LDL-HDL1 (low density lipoprotein-high density lipoprotein) and HDL1 concentrations. Compared with normally fed mice the most notable alterations in plasma lipoprotein composition were, in LDL-HDL2, greater cholesteryl ester in obese and less phospholipid in undernourished mice. In contrast, tetramethyl-urea-soluble apolipoprotein distribution was unaffected by litter size. Although moderate differences were observed in lipoprotein compositions and levels in over- or undernourished mice, further investigations of lipoprotein metabolism and metabolic abnormalities in this animal model are required. 287 NAL Call. No.: QL55.A1I43 SHHE/Mcc-cp rat: model of obesity, non-insulin-dependent diabetes, and congestive heart failure. McCune, S.A.; Baker, P.B.; Stills, H.F. Jr Washington, D.C. : Institute of Laboratory Animal Resources, National Research Council; 1990. I.L.A.R. news v. 32 (3): p. 23-27; 1990. Includes references. Language: English Descriptors: Rats; Obesity; Diabetes mellitus; Animal models; Heart diseases; Complications 288 NAL Call. No.: Z7996.P85J6 Simian & human retroviruses in nonhuman primates infection, disease & animal model studies : a bibliography, 1988-1989 annual update.. Simian and human retroviruses in nonhuman primates Johnson-Delaney, Cathy A. University of Washington, Primate Information Center Seattle, Wash. : Primate Information Center, Regional Primate Research Center, University of Washington,; 1989. 26 p. ; 28 cm. Cover title. September 1989. Supported in part by Grant No. RR-00166 from the National Institutes of Health. Includes index. Language: English Descriptors: Primates; AIDS (Disease) 289 NAL Call. No.: QR1.I57 Site-directed mutagenesis of the alpha-toxin gene of Staphylococcus aureus: role of histidines in toxin activity in vitro and in a murine model. Menzies, B.E.; Kernodle, D.S. Washington, D.C., American Society for Microbiology; 1994 May. Infection and immunity v. 62 (5): p. 1843-1847; 1994 May. Paper presented at the "33rd Interscience Conference on Antimicrobial Agents and Chemotherapy," Oct. 17-20, 1993, New Orleans, LA. Includes references. Language: English Descriptors: Staphylococcus aureus; Histidine; Toxins; Mutagenesis; Hemolysis; In vitro; Toxicity; Animal models; Mice Abstract: Staphylococcus aureus alpha-toxin is a membrane- damaging exoprotein that oligomerizes to form transmembrane pores. Chemical modification of histidines with diethylpyrocarbonate has been shown to reduce the hemolytic activity of alpha-toxin, suggesting that one or more of the histidine residues is important for toxin function. To individually assess the functional importance of each of the four histidine (residues residues 35, 48, 144, and 259), we used oligonucleotide-directed mutagenesis of the cloned alpha- toxin gene to replace each histidine with leucine. The mutant toxins were expressed in S. aureus and evaluated for hemolytic activity in vitro and for lethality in an intraperitoneal murine model. Substitution of histidine 35 with leucine produced a mutant toxin (H35L) without hemolytic or lethal activity. Mutant toxins H48L, H144L, and H259L exhibited 7, 16, and 46%, respectively, of the hemolytic activity of wild- type toxin. Immunoblotting of purified H35L toxin incubated with liposomal membranes demonstrated intact membrane binding and hexamer formation that was clearly detectable but reduced compared with that of the wild-type toxin. This suggests that hexamer formation alone is not sufficient for the expression of alpha-toxin activity. The nature of the defect underlying the lack of activity of the H35L mutant toxin remains to be elucidated but may involve failure of the hexamer to span the lipid bilayer to form a transmembrane pore or a change in the internal surface and permeability characteristics of the pore. 290 NAL Call. No.: QL698.C7 The Smyth chicken: a model for autoimmune amelanosis. Smyth, J.R. Jr Boca Raton, Fla. : CRC Press; 1989. Critical reviews in poultry biology v. 2 (1): p. 1-19; 1989. Literature review. Includes references. Language: English Descriptors: Fowls; Mutations; Polygenic inheritance; Animal models; Melanins; Autoimmune diseases; Autoantibodies; Literature reviews 291 NAL Call. No.: RC262.C5N8 Soy intake and cancer risk: a review of the in vitro and in vivo data. Messina, M.J.; Persky, V.; Setchell, K.D.R.; Barnes, S. Hillsdale, N.J. : Lawrence Erlbaum Associates, Inc; 1994. Nutrition and cancer v. 21 (2): p. 113-131; 1994. Includes references. Language: English Descriptors: Soybean products; Carcinoma; Risk; Genistein; Estrogenic properties; Transduction; Research; Literature reviews Abstract: International variations in cancer rates have been attributed, at least in part, to differences in dietary intake. Recently, it has been suggested that consumption of soyfoods may contribute to the relatively low rates of breast, colon, and prostate cancers in countries such as China and Japan. Soybeans contain a number of anticarcinogens, and a recent National Cancer Institute workshop recommended that the role of soyfoods in cancer prevention be investigated. In this review, the hypothesis that soy intake reduces cancer risk is considered by examining relevant in vitro, animal, and epidemiological data. Soybeans are a unique dietary source of the isoflavone genistein, which possesses weak estrogenic activity and has been shown to act in animal models as an antiestrogen. Genistein is also a specific inhibitor of protein tyrosine kinases; it also inhibits DNA topoisomerases and other critical enzymes involved in signal transduction. In vitro, genistein suppresses the growth of a wide range of cancer cells, with IC50 values ranging from 5 to 40 micromolar (1-10 micrograms/ml). Of the 26 animal studies of experimental carcinogenesis in which diets containing soy or soybean isoflavones were employed, 17 (65%) reported protective effects. No studies reported soy intake increased tumor development. The epidemiological data are also inconsistent, although consumption of nonfermented soy products, such as soymilk and tofu, tended to be either protective or not associated with cancer risk; however, no consistent pattern was evident with the fermented soy products, such as miso. Protective effects were observed for both hormone- and nonhormone-related cancers. While a definitive statement that soy reduces cancer risk cannot be made at this time, there is sufficient evidence of a protective effect to warrant continued investigation. 292 NAL Call. No.: 410.9 P94 Spinal dracunculiasis in an experimentally infected ferret. Broderson, J.R.; Eberhard, M.L.; Welch, B.G.; Bandt, F.H. Cordova, Tenn. : American Association for Laboratory Animal Science; 1991 Apr. Laboratory animal science v. 41 (2): p. 180-182; 1991 Apr. Includes references. Language: English Descriptors: Ferrets; Dracunculus insignis; Disease models; Animal models; Morphology; Paralysis; Experimental infections; Spinal cord; Parasite migration 293 NAL Call. No.: 410.9 P94 Spontaneous and experimental infections in scid and scid/beige mice. Percy, D.H.; Barta, J.R. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Apr. Laboratory animal science v. 43 (2): p. 127-132; 1993 Apr. Paper presented at a conference entitled "The Scid Mouse in Biomedical and Agricultural Research," August 5-7, 1992, Guelph, Canada. Includes references. Language: English Descriptors: Mice; Mutants; Infections Abstract: Severe combined immunodeficient (scid) mice are valuable animals to study a variety of logic and disease processes. Their capacity to support multiple tissue xenografts permits these mice to be used as intermediate models for host-specific, fastidious organisms for which a small animal model has not been available previously. However, because they are unable to mount a normal immune response, they are very susceptible to a variety of primary and opportunistic microbial pathogens. Fatal, naturally occurring infections with bacteria such as Proteus mirabilis, Streptococcus viridans, and Escherichia coli have been observed. In addition, based on observations after experimental or naturally occurring viral infections, scid and scid/beige mice have been shown to be very susceptible to infections with viruses such as mouse hepatitis virus, Sendai virus, and murine respiratory virus, with resulting mortality. Of the parasitic infections, Pneumocystis carinii is a relatively common contaminant of the respiratory tracts of scid mice and may complicate research projects, particularly experimental respiratory tract infections. In view of the enhanced susceptibility of these mice to infections of this type, it is essential that they be housed under optimal conditions, which include implementing stringent management practices and a functional barrier system. 294 NAL Call. No.: QH573.N37 Spontaneous hypercholesterolemia in pigs. Attie, A.D.; Aiello, R.J.; Cooper, S.T.; Uelmen, P.J. Berlin ; New York : Springer-Verlag : c1986-; 1993. NATO ASI series. Series H, Cell biology v. 73: p. 107-112; 1993. In the series analytic: Human apolipoprotein mutants. III. Diagnosis and treatment / edited by C.R. Sirtori, G. Franceschini and B.H. Brewer Jr. Proceedings of a NATO Advanced Research Workshop held April 5-8, 1992, Limone sul Garda, Italy. Includes references. Language: English Descriptors: Pigs; Hypercholesterolemia; Haplotypes; Alleles; Apolipoproteins; Low density lipoprotein; Receptors; Binding; Animal models 295 NAL Call. No.: QL55.A1I43 The spontaneously hypercholesterolemic pig as an animal model for human atherosclerosis. Attie, A.D.; Prescott, M.F. Washington, D.C. : Institute of Laboratory Animal Resources, National Research Council; 1988. I.L.A.R. news v. 30 (4): p. 5-12. ill; 1988. Includes references. Language: English Descriptors: Pigs; Disease models; Hypercholesterolemia; Atherosclerosis; Lipids; Cholesterol; Lipoproteins; Histopathology 296 NAL Call. No.: 389.1 W892 Studies of dietary supplementation with omega 3 fatty acids in patients with rheumatoid arthritis. Kremer, J.M.; Robinson, D.R. Basel : S. Karger; 1991. World review of nutrition and dietetics v. 66: p. 367-382; 1991. In the series analytic: Health effects of omega-3 polyunsaturated fatty acids in seafoods / edited by A. Simopoulos, R. Kifer, R. Martin and S. Barlow. Literature review. Includes references. Language: English Descriptors: Rheumatoid arthritis; Eicosapentaenoic acid; Docosenoic acids; Fish oils; Supplements; Immune response; Pain; Assessment; Inflammation; Leukotrienes; Platelets; Interleukins; Mitogens; Eicosanoids; Literature reviews Abstract: The purpose of this review is to summarize briefly the investigations employing omega-3 supplements in the animal model and then more thoroughly discuss subsequent clinical investigations in patients with rheumatoid arthritis. Data on the effects of omega-3 supplements on inflammatory and immune parameters is also summarized. 297 NAL Call. No.: 448.8 P21 Studies on a murine model of congenital toxoplasmosis: vertical disease transmission only occurs in BALB/c mice infected for the first time during pregnancy. Roberts, C.W.; Alexander, J. New York, N.Y. : Cambridge University Press; 1992 Feb. Parasitology v. 104 (pt.1): p. 19-23; 1992 Feb. Includes references. Language: English Descriptors: Toxoplasma gondii; Toxoplasmosis; Vertical transmission; Congenital infection; Animal models; Mice; Chronic infections; Pregnancy 298 NAL Call. No.: QR360.A1J6 Studies on glycoprotein 13 (gp13) of equid herpesvirus 1 using affinity-purified gp13, glycoprotein-specific monoclonal antibodies and synthetic peptides in a hamster model. Stokes, A.; Corteyn, A.H.; Pullen, L.A.; Doel, T.R.; Meredith, D.M.; Killington, R.A.; Halliburton, I.W.; Whittaker, G.R.; Wheldon, L.A.; Nicolson, L. Reading : Society for General Microbiology; 1991 Apr. The Journal of general virology v. 72 (pt.4): p. 923-931; 1991 Apr. Includes references. Language: English Descriptors: Horses; Equine herpesvirus; Glycoproteins; Monoclonal antibodies; Animal models; Hamsters Abstract: Hamsters were immunized with either an affinity- purified preparation of equid herpesvirus 1 (EHV-1) glycoprotein 13 (gp13) or synthetic peptides representing three sequences within the homologous glycoprotein of EHV-4, resulting in the production of antipeptide (in the case of peptide-immunized animals) or antivirus antibodies. The sera from gp13-immunized hamsters contained antibodies which showed virus-neutralizing activity and complement-mediated antibody lysis of EHV-1-infected target cells. These hamsters were protected from EHV-1 challenge. The characteristics of a panel of anti-gp13 monoclonal antibodies (P28, P17, 14H7, 16E4 and 16H9) were assessed both in vivo and in vitro. 16E4 and P28 showed high levels of complement-mediated neutralization of virus, complement-mediated lysis of virus-infected target cells and passive protection of hamsters. Furthermore, epitope mapping studies demonstrated that this glycoprotein contains a neutralizing epitope recognized by EHV-1-immune horse serum. The data imply that gp13 has potential as a candidate antigen for a molecular vaccine. 299 NAL Call. No.: 447.8 AM3 Studies on mechanisms of hepatic insulin resistance in cafeteria-fed rats. Davidson, M.B.; Garvey, D. Bethesda, Md. : American Physiological Society; 1993 Jan. American journal of physiology v. 264 (1,pt.1): p. E18-E23; 1993 Jan. Includes references. Language: English Descriptors: Obesity; Diet; Insulin; Resistance; Fatty acids; Oxidation; Lipolysis; Hyperinsulinemia; Metabolic inhibitors; Liver; Rats Abstract: Whether hyperinsulinemia causes insulin resistance or vice versa is controversial. The development of hyperinsulinemia and insulin resistance was tracked in the cafeteria-fed rat to determine which occurred first. After 3 days of cafeteria feeding the rats were obese, manifested a small but significant decrease in fasting glucose levels, and showed no change in fasting insulin levels, basal hepatic glucose production (HGP), insulin binding to hepatic membranes, and glucose utilization during a euglycemic hyperinsulinemic clamp, but the rats did demonstrate an increased glucose disappearance rate associated with an enhanced insulin response to intra-arterial glucose and hepatic insulin resistance during the clamp. After 7 days of cafeteria feeding, the results were similar except that fasting hyperglycemia and hyperinsulinemia, an enhanced basal HGP, and decreased insulin binding developed. After 6 wk of cafeteria feeding, both hepatic and peripheral insulin resistances were present. After 7 days of cafeteria feeding in rats given streptozotocin or etomoxir, an inhibitor of free fatty acid (FFA) oxidation, hepatic insulin resistance persisted despite elimination of hyperinsulinemia and reduction of FFA oxidation. These data do not support a causal role for either hyperinsulinemia or enhanced lipolysis of hypertrophied fat stores and subsequent FFA oxidation in the liver in the development of hepatic insulin resistance in this animal model of obesity. 300 NAL Call. No.: 410.9 P94 Subcutaneous abscess due to Salmonella adelaide in a grey collie with cyclic hematopoiesis. Moazed, T.C.; Deeb, B.J.; DiGiacomo, R.F. Cordova, Tenn. : American Association for Laboratory Animal Science; 1990 Nov. Laboratory animal science v. 40 (6): p. 639-641; 1990 Nov. Includes references. Language: English Descriptors: Dogs; Salmonella; Abscesses; Hematopoiesis; Animal models; Case reports; Salmonellosis; Stress 301 NAL Call. No.: QP141.A1N88 Suppression of experimental allergic encephalomyelitis after dietary zinc deprivation in guinea pigs. Scelsi, R.; Franciotta, D.M.; Camana, C.; Savoldi, F.; Allegrini, M. Elmsford, N.Y. : Pergamon Press; 1989 Dec. Nutrition research v. 9 (12): p. 1345-1354; 1989 Dec. Includes references. Language: English Descriptors: Diet; Mineral deficiencies; Zinc; Immunology; Encephalitis; Guinea pigs Abstract: The effects of different levels of zinc (Zn) in the diet were tested in the animal model of acute experimental allergic encephalomyelitis (EAE), which is considered a prototype for cell-mediated autoimmune disease of the central nervous system (CNS). Acute EAE was induced in guinea pigs maintained with normal, high and low levels of Zn in the diet. The animals fed normal and Zn-supplemented diets showed the same survival rates; the incidence and severity of the disease was similar for both groups. Zn-deficient animals exhibited the expected symptoms of Zn deficiency and after sensitization did not develop neurological signs of EAE; some of them presented only focal inflammatory alteration in CNS. 302 NAL Call. No.: 41.8 J82 Susceptibility of Balb/c, C57/B6 and C57/B10 mice to infection with Mycobacterium paratuberculosis. Chiodini, R.J.; Buergelt, C.D. London : Academic Press; 1993 Nov. Journal of comparative pathology v. 109 (4): p. 309-319; 1993 Nov. Includes references. Language: English Descriptors: Mice; Mycobacterium paratuberculosis; Animal models 303 NAL Call. No.: QR360.A1J6 Swine-reconstituted SCID mice as a model for African swine fever virus infection. Revilla, Y.; Pena, L.; Mampaso, F.; Vinuela, E.; Martinez- Alonso, C. Reading : Society for General Microbiology; 1994 Aug. The Journal of general virology v. 75 (pt.8): p 1983-1988; 1994 Aug. Includes references. Language: English Descriptors: African swine fever virus; Mice; Animal models; Infection; Blood; Lymph nodes; Spleen; Monoclonal antibodies Abstract: Injection of swine peripheral blood mononuclear cells into mice with severe combined immunodeficiency (SCID), resulted in the stable long-term establishment of a functional swine immune system (SCID-sw). Swine immunoglobulins were present in the serum of SCID-sw mice and swine cells were detected in the blood as well as in lymph nodes and spleen using monoclonal antibodies raised against cell subpopulations. Swine lymphocytes from reconstituted SCID mice responded in vitro to specific antigens or mitogens. When SCID-sw mice were challenged with African swine fever (ASF) virus. ASF virus-infected cells were detected in blood and spleen, and antiviral antibodies and virus-specific T cells were generated. 304 NAL Call. No.: QL55.A1L3 Sympathetic auricular chondritis in rats: a model of auto- immune disease?. Meingassner, J.G. London : Royal Society of Medicine Services; 1991 Jan. Laboratory animals v. 25 (1): p. 68-78; 1991 Jan. Includes references. Language: English Descriptors: Rats; Autoimmune diseases; Markers; Ear diseases; Pathology Abstract: Following the unilateral implantation of metal ear tags in female Crl:CD(SD)BR-rats, chronic inflammatory lesions were observed in both auricles in 70% and 24% of the animals after 30 and 60 weeks, respectively. Involvement of the collateral auricles was identified only after diffuse inflammation of the ear tag-marked pinnae had developed. Histological examination revealed a multifocal granulomatous chondritis, characterized by progressive destruction of the cartilaginous plate and excessive regeneration of cartilaginous tissue. IgG and complement deposits were present in the matrix of the marginal area of regenerating cartilage and at the destruction sites of autochthonous cartilage. It is likely that the pinally-restricted chondritis was due to an autoimmune response initiated by a chronic inflammatory process at the insertion site of the ear tag. Since the respone was not due to immunity to type II collagen, this pathologic phenomenon in rats may provide a useful animal model to study autoimmunity involving other cartilaginous matrix molecules. 305 NAL Call. No.: 41.8 AM3 Systemic and pulmonary reactions in swine with endotoxemia and gram-negative bacteremia. Olson, N.C.; Kruse-Elliott, K.T.; Dodam, J.R. Schaumburg, Ill. : The Association; 1992 Jun15. Journal of the American Veterinary Medical Association v. 200 (12): p. 1870-1884; 1992 Jun15. Includes references. Language: English Descriptors: Pigs; Circulatory disorders; Endotoxins; Toxemia; Gram negative bacteria; Bacterial diseases; Literature reviews; Physiopathology; Animal models 306 NAL Call. No.: QL55.A1L3 Systemic histopathology of rats with CCl(4)-induced hepatic cirrhosis. Doi, K.; Kurabe, S.; Shimazu, N.; Inagaki, M. London : Royal Society of Medicine Services; 1991 Jan. Laboratory animals v. 25 (1): p. 21-25; 1991 Jan. Includes references. Language: English Descriptors: Rats; Carbon tetrachloride; Histopathology; Animal models; Disease models; Cirrhosis Abstract: Systemic histopathological examinations were carried out on rats with CCl4-induced hepatic cirrhosis. Moderate congestion in the spleen, prominent oedema and focal acinar cell degeneration in the pancreas, marked haemorrhage and phagocytosis of haemosiderin by macrophages in the pancreaticoduodenal lymph node, appearance of monocytes bearing haemosiderin-like granules in the pulmonary arteries and cardiac right atrium, and focal segmental glomerulosclerosis were consistently observed in rats with hepatic cirrhosis. In addition, a marked increase in number of target cells and the appearance of a small number of monocytes bearing haemosiderin-like granules were also commonly found in the peripheral blood smears of these animals. These findings are considered to be important in the use of the CCl4-induced model of hepatic cirrhosis in the rat. 307 NAL Call. No.: QR1.I57 T-lymphocyte response in a guinea pig model of tuberculous pleuritis. Phalen, S.W.; McMurray, D.N. Washington, D.C. : American Society for Microbiology; 1993 Jan. Infection and immunity v. 61 (1): p. 142-145; 1993 Jan. Includes references. Language: English Descriptors: Guinea pigs; Animal models; Tuberculosis Abstract: The ability to induce tuberculous pleuritis in Mycobacterium bovis BCG-vaccinated guinea pigs was investigated as a model of human disease. A pleural effusion of 5 to 10 ml was obtained 6 to 7 days after the bilateral pleural injection of a suspension of heat-killed M. tuberculosis cells. Histological lesions were indicative of granulomatous pleuritis. Comparative studies of T lymphocytes obtained from pleural fluid and peripheral blood revealed increased antigen-driven lymphoproliferation and E rosette formation in pleural effusion lymphocytes. The CD2+ T- lymphocyte population appeared to be expanded or concentrated in pleural fluid, suggesting a compartmentalization of antigen-reactive T lymphocytes. These data demonstrate that experimental tuberculous pleuritis with effusion, closely resembling the human disease, can be produced in BCG- vaccinated guinea pigs. 308 NAL Call. No.: RC347.5.T69 1994 Toxin-induced models of neurological disorders. Woodruff, Michael L.; Nonneman, Arthur J. New York : Plenum Press,; 1994. xxi, 344 p. : ill. ; 24 cm. Includes bibliographical references and index. Language: English Descriptors: Neurotoxicology; Nervous system 309 NAL Call. No.: 470 SCI2 Transgenic animals. Jaenisch, R. Washington, D.C. : American Association for the Advancement of Science; 1988 Jun10. Science v. 240 (4858): p. 1468-1474; 1988 Jun10. Literature review. Includes references. Language: English Descriptors: Mice; Gene expression; Genetic engineering; Genomes; Disease models; Neoplasms Abstract: Astract: The ability to introduce foreign genes into the germ line and the successful expression of the inserted gene in the organism have allowed the genetic manipulation of animals on an unprecedented scale. The information gained from the use of the transgenic technology is relevant to almost any aspect of modern biology including developmental gene regulation, the action of oncogenes, the immune system, and mammalian development. Because specific mutations can be introduced into transgenic mice, it becomes feasible to generate precise animal models for human genetic diseases and to begin a systematic genetic dissection of the mammalian genome. 310 NAL Call. No.: 500 N21P Transgenic mice overexpressing phosphoenolpyruvate carboxykinase develop non-insulin-dependent diabetes mellitus. Valera, A.; Pujol, A.; Pelegrin, M.; Bosch, F. Washington, D.C. : National Academy of Sciences,; 1994 Sep13. Proceedings of the National Academy of Sciences of the United States of America v. 91 (19): p. 9151-9154; 1994 Sep13. Includes references. Language: English Descriptors: Mice; Experimental diabetes; Diabetes; Diabetes mellitus; Transgenic animals; Gene transfer; Phosphoenolpyruvate carboxykinase; Gene expression; Gluconeogenesis; Liver; Hyperglycemia; Glucose; Carbohydrate metabolism; Liver cells Abstract: An increase in hepatic gluconeogenesis is believed to be an important factor responsible for the fasting hyperglycemia detected in patients with non-insulin-dependent diabetes mellitus (NIDDM). Phosphoenolpyruvate carboxykinase (GTP) (PEPCK; EC 4.1.1.32) is a regulatory enzyme of gluconeogenesis. To study the role of the expression of PEPCK gene in the development of NIDDM, we have produced lines of transgenic mice expressing a PEPCK minigene under control of its own promoter. Transgenic mice were hyperglycemic and had higher serum insulin concentrations. In addition, alterations in liver glycogen content and muscle glucose transporter GLUT-4 gene expression were detected. The overexpression of the PEPCK gene led to an increase in glucose production from pyruvate in hepatocytes in primary culture. When intraperitoneal glucose tolerance tests were performed, blood glucose levels were higher than those detected in normal mice. This animal model shows that primary alterations in the rate of liver glucose production may induce insulin resistance and NIDDM. 311 NAL Call. No.: 448.3 AC85 Treatment of bovine leukaemia virus-infected sheep with suramin: an animal model for the development of antiretroviral compounds. Burkhardt, H.; Rosenthal, S.; Rosenthal, H.A.; Karge, E.; De Clercq, E. Praha : Academia, Publishing House of the Czechoslovak Academy of Sciences; 1989 Aug. Acta virologica v. 33 (4): p. 305-313; 1989 Aug. Includes references. Language: English Descriptors: Bovine oncovirus; Sheep; Drug therapy; Suramin; Models; Enzyme activity 312 NAL Call. No.: QP901.A33 Trophic stimulation of the ductular-islet cell axis: a new approach to the treatment of diabetes. Rosenberg, L.; Vinik, A.I. New York, N.Y. : Plenum Press; 1992. Advances in experimental medicine and biology v. 321: p. 95-109; 1992. In the series analytic: Pancreatic islet cell regeneration and growth / edited by A.I. Vinik. Proceedings of the Diabetic Institute Conference on Inslet Cell Regeneration and Growth, June 22-23, 1991, Norfolk, Virginia. Includes references. Language: English Descriptors: Diabetes mellitus; Pancreas islets; Cell differentiation; Cell growth; Regeneration; Animal models; Golden hamsters 313 NAL Call. No.: 41.8 J82 Tuberculosis in domesticated deer (Cervus elaphus): a large animal model for human tuberculosis. Buchan, G.S.; Griffin, J.F.T. London : Academic Press; 1990 Jul. Journal of comparative pathology v. 103 (1): p. 11-22. ill; 1990 Jul. Includes references. Language: English Descriptors: Red deer; Mycobacterium bovis; Histopathology; Immunodiagnosis; Lymphocyte transformation tests; Elisa; Skin tests; Stress; Immunological deficiency; Disease models; Animal models 314 NAL Call. No.: 500 N21P Tumor necrosis factor alpha inhibits signaling from the insulin receptor. Hotamisligil, G.S.; Murray, D.L.; Choy, L.N.; Spiegelman, B.M. Washington, D.C. : National Academy of Sciences,; 1994 May24. Proceedings of the National Academy of Sciences of the United States of America v. 91 (11): p. 4854-4858; 1994 May24. Includes references. Language: English Descriptors: Mice; Tumor necrosis factor; Insulin; Hormone receptors; Phosphorylation; Hormonal control; Adipocytes; Glucose; Active transport; Diabetes mellitus Abstract: Insulin resistance is a common problem associated with infections and cancer and, most importantly, is the central component of non-insulin-dependent diabetes mellitus. We have recently shown that tumor necrosis factor (TNF) alpha is a key mediator of insulin resistance in animal models of non-insulin-dependent diabetes mellitus. Here, we investigate how TNF-alpha interferes with insulin action. Chronic exposure of adipocytes to low concentrations of TNF-alpha strongly inhibits insulin-stimulated glucose uptake. Concurrently, TNF- alpha treatment causes a moderate decrease in the insulin- stimulated autophosphorylation of the insulin receptor (IR) and a dramatic decrease in the phosphorylation of IR substrate 1, the major substrate of the IR in vivo. The IR isolated from TNF-alpha-treated cells is also defective in the ability to autophosphorylate and phosphorylate IR substrate 1 in vitro. These results show that TNF-alpha directly interferes with the signaling of insulin through its receptor and consequently blocks biological actions of insulin. 315 NAL Call. No.: 41.8 P27 Ultraviolet radiation-induced skin tumors in a South American opossum (Monodelphis domestica). Kusewitt, D.F. Lawrence, Kan. : American College of Veterinary Pathologists; 1991 Jan. Veterinary pathology v. 28 (1): p. 55-65. ill; 1991 Jan. Includes references. Language: English Descriptors: Monodelphis domestica; Skin diseases; Neoplasms; Ultraviolet radiation; Histopathology; Sarcoma; Melanoma; Papillomas; Carcinoma; Animal models; Disease models 316 NAL Call. No.: SF95.A1C6 v.6 Use of animal models for research in human nutrition. Beynen, Anton C.,_1953-; West, C. E. Basel ; New York : Karger,; 1988. 190 p. ; 25 cm. (Comparative animal nutrition ; v. 6). Includes bibliographies and index. Language: English Descriptors: Nutritionally induced diseases; Animal models; Animal nutrition 317 NAL Call. No.: SF95.A1C6 Use of animals for the study of relations between nutrition and infectious diseases. Beisel, W.R. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 33-55; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Literature review. Includes references. Language: English Descriptors: Animal models; Malnutrition; Infectious diseases; Fatal infections; Mineral deficiencies; Synergism; Antagonism; Species differences; Pathogens; Strain differences; Vitamin deficiencies; Deficiency diseases; Immune response; Endotoxins; Literature reviews 318 NAL Call. No.: SF95.A1C6 Use of animals in elucidating the regulation of metabolism of amino acids with particular reference to branched chain amino acids. Goodwin, G.W.; Harris, R.A. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 14-30; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Literature review. Includes references. Language: English Descriptors: Rats; Animal models; Amino acid metabolism; Branched chain amino acids; Catabolism; Oxidoreductases; Enzyme activity; Dietary protein; Liver cells; Biotechnology; Dna probes 319 NAL Call. No.: RC372.3.S5 The use of animals in research related to epilepsy and other disorders in which convulsions may occur. Silcock, Sheila Sussex, UK? : RSPCA,; 1989. 49 p. ; 30 cm. Cover title. August 1989. Includes bibliographical references (p. 44-49). Language: English Descriptors: Epilepsy; Animal models in research; Convulsions 320 NAL Call. No.: SF95.A1C6 The use of animals in studying the effects of diet on gallstone formation. Liepa, G.U.; Gorman, M.A.; Duffy, A.M. Basel : Karger; 1988. Comparative animal nutrition v. 6: p. 149-173; 1988. In the series analytic: Use of Animal Models for Research in Human Nutrition / edited by A.C. Beynen and C.E. West. Includes references. Language: English Descriptors: Animal models; Biliary calculi; Bile; Hamsters; Cholesterol metabolism; Dietary protein; Blood serum; Laboratory animals; Mice; Dietary fat; Primates 321 NAL Call. No.: QD415.A1B58 The use of gene targeting to develop animal models for human genetic diseases. Melton, D.W. Colchester : The Society; 1990 Dec. Transactions - Biochemical Society v. 18 (6): p. 1035-1039. ill; 1990 Dec. Includes references. Language: English Descriptors: Transgenics; Genetic engineering; Animals; Models; Genetic disorders; Therapy 322 NAL Call. No.: R853.A53U84 1989 The use of laboratory animals in biomedical research significance for human and animal health : information package.. Information package; the use of laboratory animals in biomedical research National Association for Biomedical Research (U.S.) Washington : DC? : National Association for Biomedical Research?,; 1989. 174 p. : ill. ; 28 cm. Cover title. January 1989. Includes bibliographical references. Language: English Descriptors: Animal experimentation; Animal models in research; Medicine; Diseases; Animal welfare 323 NAL Call. No.: 448.3 Ap5 Virulence of an Escherichia coli O157:H7 sorbitol-positive mutant. Fratamico, P.M.; Buchanan, R.L.; Cooke, P.H. Washington : American Society for Microbiology; 1993 Dec. Applied and environmental microbiology v. 59 (12): p. 4245-4252; 1993 Dec. Includes references. Language: English Descriptors: Escherichia coli; Sorbitol; Carbohydrate metabolism; Fermentation; Mutants; Virulence; Pathogenicity; Experimental infections; Rabbits; Diarrhea; Foodborne diseases; Pathogens Abstract: Virulence and pathogenicity of an Escherichia coli O157:H7 sorbitol-positive mutant were investigated with an infant rabbit animal model as well as a battery of in vitro assays. Total cell lysate protein profiles, outer membrane protein profiles, plasmid profiles, and levels of cytotoxic activity against Vero cells were similar in the wild-type and mutant strains. Both adhered to intestinal epithelial cells in culture and reacted with fluorescein isothiocyanate-labeled antiserum against E. coli O157:H7. The mutant appeared to be similar to the wild type in all respects except in its ability to ferment sorbitol. [14C]sorbitol uptake and sorbitol-6- phosphate dehydrogenase activities were notably increased in the mutant strain. Diarrhea developed in rabbits administered the wild-type strain and in those fed the sorbitol-positive mutant. There was greater bacterial attachment and mucosal damage in the cecum and large intestine than in the small intestine. Scanning electron microscopy revealed bacteria adhering as single cells and as aggregates closely associated with mucus. Mucosal lesions consisted of areas of tissue necrosis with sloughing of epithelial cells. By transmission electron microscopy, electron-dense necrotic epithelial cells were visible in areas where bacteria were present, and epithelial cell debris containing bacteria was observed between the villar luminal surfaces. Light microscopy of epithelial cells of intestinal sections of infected rabbits revealed noticeable vacuolation and spherical, pyknotic nuclei. These data indicate that the sorbitol-negative phenotype is not associated with the pathogenicity of E. coli O157:H7. 324 NAL Call. No.: 500 N21P Vitamin C prevents cigarette smoke-induced leukocyte aggregation and adhesion to endothelium in vitro. Lehr, H.A.; Frei, B.; ARfors, K.E. Washington, D.C. : National Academy of Sciences,; 1994 Aug02. Proceedings of the National Academy of Sciences of the United States of America v. 91 (16): p. 7688-7692; 1994 Aug02. Includes references. Language: English Descriptors: Hamsters; Ascorbic acid; Protection; Tobacco smoking; Cigarettes; Smoke; Leukocytes; Adhesion; Endothelium; Blood vessels Abstract: A common feature of cigarette-smoke (CS)-associated diseases such as atherosclerosis and pulmonary emphysema is the activation, aggregation, and adhesion of leukocytes to micro- and macrovascular endothelium. A previous study, using a skinfold chamber model for intravital fluorescence microscopy in awake hamsters, has shown that exposure of hamsters to the smoke generated by one research cigarette elicits the adhesion of fluorescently labeled leukocytes to the endothelium of arterioles and small venules. By the combined use of intravital microscopy and scanning electron microscopy, we now demonstrate in the same animal model that (i) CS-induced leukocyte adhesion is not confined to the microcirculation, but that leukocytes also adhere singly and in clusters to the aortic endothelium; (ii) CS induces the formation in the bloodstream of aggregates between leukocytes and platelets; and (iii) CS-induced leukocyte adhesion to micro- and macrovascular endothelium and leukocyte-platelet aggregate formation are almost entirely prevented by dietary or intravenous pretreatment with the water-soluble antioxidant vitamin C (venules, 21.4 +/- 11.0 vs. 149.6 +/- 38.7 leukocytes per mm(2), P < 0.01; arterioles, 8.5 +/- 4.2 vs. 54.3 +/- 21.6 leukocytes per mm(2),P < 0.01; aortas, 0.8 +/- 0.4 vs. 12.4 +/- 5.6 leukocytes per mm(2), P < 0.01; means +/- SD of n = 7 animals, 15 min after CS exposure). No inhibitory effect was observed by pretreatment of the animals with the lipid-soluble antioxidants vitamin E or probucol. The protective effects of vitamin C on CS-induced leukocyte adhesion and aggregation were seen at vitamin C plasma levels (55.6 +/- 22.2 micromolar, n = 7) that can easily be reached in humans by dietary means or supplementation, suggesting that vitamin C effectively contributes to protection from CS- associated cardiovascular and pulmonary diseases in humans. 325 NAL Call. No.: 500 N484 Vitamin E and cancer prevention in an animal model. Wang, Y.M.; Purewal, M.; Nixon, B.; Li, D.H.; Soltysiak- Pawluczuk, D. New York, N.Y. : The Academy; 1989. Annals of the New York Academy of Sciences v. 570: p. 383-390; 1989. In the series analytic: Vitamin E--biochemistry and health implications / edited by A.T. Diplock, L.J. Machlin, L. Packer and W.A. Pryor. Includes references. Language: English Descriptors: Carcinoma; Diet studies; Disease prevention; Disease surveys; Vitamin e; Human nutrition research; Rats 326 NAL Call. No.: 389.1 W892 Vitamins and hypertension. Dakshinamurti, K.; Lal, K.J. Basel : S. Karger; 1992. World review of nutrition and dietetics v. 69: p. 40-73; 1992. In the series analytic: Nutrients in the control of metabolic diseases / edited by A.P. Simopoulos. Includes references. Language: English Descriptors: Hypertension; Pyridoxine; Vitamin d; Vitamin e; Vitamin deficiencies; Blood pressure; Animal models; Calcium; Nutrition physiology; Literature reviews Abstract: Based on the evidence presented in this review, the authors offer the following conclusions: 1) Among the vitamins, pyridoxine and cholecalciferol seem to have significant influences on blood pressure regulation. 2) The effect of vitamin E seems to be indirect based on the maintenance of integrity of membranes. 3) Vitamin D is directly involved in regulation of calcium homeostasis. Conditions associated with a deficiency of vitamin D or its conversion to the active form, would have profound effect on calcium absorption and, thus, indirectly on regulation of blood pressure. 327 NAL Call. No.: 500 N484 Vitamins and the immune system. Beisel, W.R. New York, N.Y. : The Academy; 1990. Annals of the New York Academy of Sciences v. 587: p. 5-8; 1990. In the series analytic: Micronutrients and immune functions / edited by A. Bendich and Ranjit K. Chandra. Includes references. Language: English Descriptors: Ascorbic acid; Pyridoxine; Retinol; Vitamin e; Human nutrition research; Immune response; Immunology; Trace elements; Mice; Animal models 328 NAL Call. No.: 442.9 SO1 Vitamin A status: relationship to immunity and the antibody response. Ross, A.C. Baltimore, Md. : Williams & Wilkins; 1992 Jul. Proceedings of the Society for Experimental Biology and Medicine v. 200 (3): p. 303-320; 1992 Jul. Literature review. Includes references. Language: English Descriptors: Retinol; Retinoic acid; Vitamin a deficiency; Cell mediated immunity; Humoral immunity; Antibody formation; Antigens; Natural killer cells; Infections; Immunization; Animal models; Literature reviews 329 NAL Call. No.: 389.8 J82 Weanling rats display bioperiodicity of growth and food intake rates. Mercer, L.P.; Haijazi, H.; Hidevgi, M. Bethesda, Md. : American Institute of Nutrition; 1993 Aug. The Journal of nutrition v. 123 (8): p. 1356-1362; 1993 Aug. Includes references. Language: English Descriptors: Growth; Growth rate; Biological rhythms; Casein; Valine; Methionine; Weight gain; Experimental diets; Animal models; Rats Abstract: Bioperiodicities in biological phenomena have long been studied to gain insight into the dynamics of living organisms. However, apparent periodicities in rates of growth and food intake have often been either ignored or attributed to random error. We have found that such periodicities are not random but take the form of infradian rhythms (period > 28 h), with multiple periods including circasemiseptan (period = 3.5 d). in the reported experiments, we examine the existence of periodic, oscillatory phenomena in growth and eating patterns of rats. The cosinor model of Halberg was used to establish the occurrence of rhythms and quantify rhythm characteristics of components identified in least squares spectra. The four parameters of the rhythm were found to be altered by concentrations of the limiting dietary nutrient in that they had different spectral signatures. Existence of such oscillations in growth rates and food intake rates could have important consequences in designing feeding and growth experiments for achieving optimal physiological responses as well as providing possible insights into eating disorders. 330 NAL Call. No.: 410.9 P94 Xenogeneic PBL-scid mice: their potential and current limitations. Greenwood, J.D. Cordova, Tenn. : American Association for Laboratory Animal Science; 1993 Apr. Laboratory animal science v. 43 (2): p. 151-155; 1993 Apr. Paper presented at a conference entitled "The Scid Mouse in Biomedical and Agricultural Research," August 5-7, 1992, Guelph, Canada. Includes references. Language: English Descriptors: Animal models; Mice; Lymphocytes Abstract: The hu-PBL-scid has been constructed by intraperitoneal inoculation of lymphocytes from human peripheral blood into immunodeficient scid mice. Such scid mouse-human chimeras have proven useful as in vivo animal models for studies on human lymphocyte development and differentiation from pluripotent stem cells. Further, the hu- PBL-scid mouse provides a readily accessible model for the examination of immune cell function and involvement in autoimmune and infectious disease processes. In response to the growing need for model systems to examine the immune system and disease pathogenesis in agriculturally important animals, PBL engraftment of scid mice has expanded to include the bovine and equine species. This review discusses the properties and potential uses of the xenogeneic PBL- reconstituted scid mouse.
Abileah, S. 222 Ackermann, M.R. 185 Adams, J.L. 234 Adams, Robert J. 150 Adlam, C. 23 Ahern-Rindell, A.J. 249 Aiello, R.J. 294 Ailhaud, G. 245 Albertini, A. 250 Alder, V.A. 79 Alexander, J. 297 Allegrini, M. 301 Allen, G.P. 171 Alziari, S. 225 Amy, R.M. 208, 270 Aoki, F.Y. 67 Apgar, J. 269 Arai, T. 189 Arbeeny, C.M. 122 Arendonk, J.A.M. van 114 ARfors, K.E. 324 Arp, L.H. 148 Asano, T. 66 Attie, A.D. 294, 295 Aubert, R. 286 Aukema, H.M. 127 Austin, L.L. 194 Austin-Lafrance, R.J. 261 Azmi, M. 201 Bacchus, C. 48 Bacon, W.L. 64 Baker, George T. 260 Baker, P.B. 287 Bandt, F.H. 292 Bannatyne, R.M. 231 Barbee, D.D. 267 Barnes, S. 291 Barr, R.J. 74 Barr, S.C. 136 Barrett, D.S. 115 Barrett-Connor, E. 103 Barsh, G.S. 244 Barta, J.R. 293 Basson, N.J. 143 Baumal, R. 56 Bautista, J.R. 49 Beard, J.L. 52, 235 Beatty, R.J. 167 Beausoleil, N. 156 Beisel, W.R. 317, 327 Bell, J.D. 195 Bell, J.G. 121 Belton, P.S. 195 Berdanier, C.D. 95 Bergquist, K.E. 122 Beynen, A.C. 65 Beynen, Anton C., 108 Beynen, Anton C.,_1953- 316 Beziat, F. 225 Bhathena, S.J. 119, 277 Bishop, S.A. 149 Blanchette-Mackie, E.J. 93 Blenden, D.C. 223 Blondeau, J.M. 67 Bloom, F.E. 236 Bodo, M. 160 Boffa, G.M. 250 Bohnsack, J.F. 275 Boothe, D.M. 111 Boothe, H.W. 111 Bosch, F. 310 Bosshard, N.U. 157 Bourgeois, F. 286 Bourque, W.T. 273 Bovee, K.C. 217 Bradley, A. 184 Bray, G.A. 252 Brennan, M.F. 13 Breslow, J. 210 Bridenstine, R.T. 133 Briner, J. 157 Broderson, J.R. 292 Bronzino, J.D. 261 Brown, F. 166 Bruss, M.L. \u University of California, Davis, CA 219 Buchan, G.S. 313 Buchanan, R.L. 323 Buergelt, C.D. 302 Bunch, T. 166 Burgin, C.W. 167 Burkhardt, H. 311 Burns, R.A. 121 Burny, A. 50 Buselmaier, W. 48 Butler, D.G. 147 Butterworth, R.F. 263 Byham, L.D. 100 Calnek, B.W. 70 Camana, C. 301 Camus, M.C. 286 Cantor, Jerome O. 88 Capellan, J.M. 231 Capodicasa, E. 71 Carapetis, R. 14 Carbone, K.M. 49 Caroldi, S. 71 Carraway, J.H. 209 Carroll, K.K. 278 Carswell, N. 119 Carter, J.W. 144 Caskey, C.T. 184 Cerda, J.J. 167 Cha, Y.S. 58 Chambon, C. 36 Chang, J.K. 275 Chao, F.F. 93 Charnock, J.S. 38 Chastin, I. 36 Cheevers, W.P. 267 Chen, M.L. 222 Chen, M.T. 130 Cheng, P. 231 Chiodini, R.J. 302 Chowdhury, J.R. \u Albert Einstein College of Medicine, Bronx, NY 170 Chowdhury, N.R. 170 Choy, L.N. 314 Christman, J.K. 222 Chu, H. 69 Ciresi, R. 173 Clabough, D.L. 152 Clark, A.M. 113 Clarkson, R.B. 82 Clarkson, T.B. 26 Clifford, A.J. 116 Clingerman, K. 28 Coates, F. 156 Coghlan, L. 174 Cohen, L.A. 268 Conboy, H.S. 152 Condorelli, E. 250 Conner, B.H. 110 Connolly, J.M. 104 Connor, J.D. 52 Connor, W.E. 141 Contreras, R.J. 107 Cooke, P.H. 323 Cooley, A.J. 234 Cooper, D.R. 200 Cooper, S.T. 294 Cornelius, C.E. 154 Cornelius, C.E. \u University of California, Davis, CA 153 Cornelius, Charles E. 22 Corrier, D.E. 111 Corteyn, A.H. 298 Cotsonis, G.A. 227 Cotter, P.A. 54 Cox, I.J. 195 Crabble, J.C. 162 Cranwell, P.D. 257 Cray, W.C. Jr 37 Cremer, K.J. 35 Cringle, S.J. 79 Crusberg, T.C. 140 Cruse, Julius M.,_1937- 62 Cullen, J.M. 111 Curello, S. 250 Cyr, D. 263 Czuprynski, C.J. 234 D'Aquino, M. 118 Dakshinamurti, K. 326 Daley, E. 156 Daoust, L. 202 Davidson, M.B. 299 Davis, N.L. 42 De Clercq, E. 311 Dean, E.A. 148 DeCarli, L.M. 25 Deeb, B.J. 300 Deming, E.J. 15 DeRousseau, C. Jean 248 Deyl, Zdenek 221 Di Felice, M. 118 Diamond, Herbert S., 87 Dickens, B.F. 93 Dietrich, H.M. 181 Dietschy, J.M. 271 DiGiacomo, R.F. 300 DiGirolamo, M. 227 Diker, F.S. 146 Diker, K.S. 146 Dionne, S. 202 Dizik, M. 222 Dodam, J.R. 305 Doel, T.R. 298 Doi, K. 306 Dolphin, P.J. 270 Donovan, S.M. \u University of Illinois, Urbana, IL 169 Dooley, T.P. 142 Douglas, S.D. 243 Doyle, R.E. 233 Dubielzig, R.R. 61 Dubreuil, J.D. 262 Duffy, A.M. 320 Dukes, I.D. 89 Dulin, A. 269 Dunaway, G.A. 94 Easter, R.A. 203 Eberhard, M.L. 292 Edelsteinova, S. 131 Efendic, S. 192 Elder, J.H. 236 Elliott, S.C. 223 Engstrand, L. 199 Erdmann, G. 206 Esparza, J. 17 Evermann, J.F. 77 Farber, J.M. 156 Farese, R.V. 200 Faribrother, J.M. 262 Faustman, D. 2 Fearon, K.C.H. 215 Feingold, K.R. 282 Fenstermacher, E.A. 217 Fernandes, G. 281 Ferrari, R. 250 Ferre, P. 91 Fettman, M.J. 9 Field, H.J. 201 Findon, G. 255 Fishlock, R.C. 14 Fisler, J.S. \u University of California, Los Angeles, CA 53 Focht, S.J. 164 Fong, I.W. 231 Ford, C.W. 135 Fosmire, G.J. 164 Fournier, J. 156 Fowke, J.H. 198 Fox, H.S. 236 Fragonas, E. 137 Fraker, P. 242 Fraker, P.J. 191 Franciotta, D.M. 301 Frangakis, C.J. 89 Fratamico, P.M. 323 Freedland, R.A. 154 Freeman, A.E. 272 Frei, B. 324 Freinkel, N. 97 Friedlander, N.J. 103 Friedman, A. 193 Frigeri, L.G. 244 Fu, Y. 2 Fukui, M. 66 Fukumoto, H. 211 Gabriel, E. 160 Gabrielson, D.A. 78 Galler, J. 261 Gamble, W. 93 Garofalo, C. 202 Garvey, D. 299 Garvy, B.A. 191 Gavin, P.R. 267 Gentili, V. 118 Gerlach, R.F. 7 Geske, R. 184 Gibson, B.M. 143 Giebink, G.S. 206 Giguere, R. 263 Gilbert, R.O. 185 Gill, A.M. 244 Gillett, N.A. 7 Gitzelmann, R. 157 Glade, M.J. 129 Glavin, G.B. 67 Glowa, J. 4 Gluckman, J. C. 32 Gnudi, L. 5 Godeas, C. 137 Gold, P.W. 4 Goodwin, G.W. 318 Gorman, M.A. 320 Goto, N. 196 Gragtmans, N.J. 220 Granato, D. 83 Grand, R.J. 182 Grandolfo, M. 137 Grant, G.L. 152 Grant, K.A. 44 Green, R.A. 111 Greenberg, E.R. 276 Greenwald, G.F. 42 Greenwald, Robert A.,_1943- 87 Greenwel, P. 34 Greenwood, J.D. 330 Griffin, C.E. 74 Griffin, J.F.T. 313 Gross, M. 273 Gruber, J. 35 Grunfeld, C. 282 Guarnieri, G. 250 Guberski, D.L. 96 Guo, J. 2 Guo, Z.M. 63, 265 Gustavsson, S. 199 Guthrie, M.J. 116 Gwathmey, J.K. 229 Haijazi, H. 329 Hall, B.K. 273 Hall-Craggs, M. 232 Halliburton, I.W. 298 Halsted, C.H. 8, 73 Hamilton, H.L. 234 Hampson, D.J. 254 Hancock, M.L. 125 Hansen, C. 277 Hansen, C.T. 92, 119, 213 Hansen, R.J. \u University of California, Davis, CA 43 Hara, C. 155 Hara, K.S. 256 Harada, T. 266 Harris, M.C. 243 Harris, R.A. 318 Harvey, J.W. 94 Haskins, M.E. 176 Hayden, J.E. 176 Hayes, K.C. 106 Haziroglu, R. 146 Hegstad, R.L. 9 Heisler, O.R. 208 Hendrickx, A.G. 121 Heng, J. 132 Henriksen, S.J. 236 Herberg, L. 16 Herndon, M.W. 271 Herzog, J. 286 Hetzel, B.S. 279 Hidevgi, M. 329 Higgins, B. 233 Hill, H.R. 275 Hirose, H. 45 Ho, C.C. 116 Ho, Y.K. 116 Hoeg, J.M. 1 Hollifield, V. 213 Holmes, R.A. 136 Holub, B.J. 127 Hope, J. 195 Horzinek, Marian C. 18 Hosie, M.J. 90 Hosokawa, S. 238 Hotamisligil, G.S. 314 How, S.J. 123 Howard, R.B. 69 Hsu, B.Y.L. 217 Huang, L.C. 200 Huether, G. 12 Hufford, C.D. 113 Hyun, B.H. 237 Iglauer, Franz 138 Ikeda, H. 3, 211 Imura, H. 211 Inagaki, M. 306 Ingram, Donald K. 260 Institute of Laboratory Animal Resources (U.S.), Committee on Immunologically Compromised Rodents 188 Inui, K. 266 Inzana, T.J. 186 Ip, C. 84 Itakura, C. 168 Ito, K. 85 Jackson, W.D. 182 Jaenisch, R. 309 Janig, W. 145 Jayo, J.M. 128 Jenkins, W.L. 111 Jevcak, J.J. 220 Jezyk, P.F. 176 Jiao, S. 3 Johnson, B.J.B. 42 Johnson, D.E. 232 Johnson, J.H. 45 Johnson, R. 51 Johnson-Delaney, Cathy A. 288 Johnston, M.R. 69 Johnston, R.E. 42 Johnston, S.D. 9 Jones, B.C. 52 Jones, J. 119 Jones, P. 184 Jones, P.W. 254 Jorgensen, A. 199 Kahn, B.B. 5 Kamimura, E. 134 Kanarek, R.B. 24, 109 Kanety, H. 183 Kaplan, J.R. 128 Karasik, A. 183 Karge, E. 311 Kasahara, K. 205 Kasai, N. 134 Katoh, T. 168 Kaufman, L.N. 130 Kausche, F.M. 148 Kawaguchi, A. 238 Kawaoka, Y. 139 Kayyali, U.S. 198 Keen, C.L. 121 Kehrli, M.E. Jr 185, 272 Kelley, D.H. 272 Kennedy, B.W. 119 Kerkhofs, P. 50 Kernodle, D.S. 289 Kettmann, R. 50 Khan, A. 192 Khosla, P. 106 Killington, R.A. 298 Kinebuchi, H. 117 King, L.E. 191 King, S. 107 Klei, T.R. 136 Kliegman, R.M. 132 Klimes, I. 131 Klumpp, S.A. 82 Knowles, D.P. 267 Koeslag, D.G. 207, 270 Koh, G. 211 Kondapalli, R. 170 Konietzko, S. 206 Koo, S.I. 144 Korpela, H. 175 Koskela, M. 206 Kovacsova, B. 131 Kozarsky, K.F. 194 Kramer, T. 269 Kremer, J.M. 296 Krinsky, N.I. 60 Kristek, F. 131 Kritchevsky, D. 98 Kruse-Elliott, K.T. 305 Kruth, H.S. 93 Kubo, M. 3 Kumazawa, A. 85 Kurabe, S. 306 Kurata, K. 126 Kurihara, K. 85 Kuriyama, M. 165 Kuroda, J. 168 Kusewitt, D.F. 315 Kutner, M.H. 227 Kuznetsov, A. 89 Kvam, B.J. 137 Kyselovic, J. 131 Laboratory Animals Information Service Centre (India) 19 Lacy, P.E. 177 Ladiges, W.C. 10, 55 Ladiges, W.C. \u University of Washington, Seattle, WA 11 Lal, K.J. 326 Lallier, R. 262 Lancaster, M.E. 89 Lariviere, S. 262 Larner, J. 200 Larson, J.A. 29 Leach, F. 5 Lee, Y. 45, 112 LeFebvre, R.B. 264 Lehr, H.A. 324 Leiter, E.H. 240 Lemonnier, D. 286 Lepage, G. 202 Lerner, D.L. 236 Letvin, Norman L. 32 Levander, O.A. 285 Levine, J.F. 152 Levy, E. 202 Lewis, R. E. 62 Lewis, S.M. 209 Li, D.H. 325 Li, F. 2 Licinio, J. 4 Lieber, C.S. 25 Liepa, G.U. 320 Limoges, B.F. 270 Litschi, B. 157 Liu, C.T. 63, 265 Lloyd, D.H. 123 Lockatell, C.V. 232 Lonnerdal, B. 121 Lotti, M. 71 Lowseth, L.A. 7 Lucke, V.M. 149 Lund, A. 190 Lunenfeld, B. 183 Lusis, A.J. 53 Luskey, K.L. 112 Lust, G. 258 Lutz, H. 157 Luzarraga, M.B. 280 Lysons, R.J. 254 M.D. Anderson Cancer Center, Science-Park Research Division 230 Maeda, H. 68, 205 Mahoney, S.G. 217 Maita, K. 266 Makar, A.B. 159 Mammerickx, M. 50 Mampaso, F. 303 Mannen, H. 196 Mano, M.T. 279 Manuck, S.B. 128 Marcell, T. 69 Marks-Kaufman, R. 24 Marlar, A.B. 61 Marrano, P. 56 Marsh, P.A. 119 Martinez-Alonso, C. 303 Mason, P.W. 166 Masoro, E.J. 241 Masuda, K. 211 Matsubara, K. 3 Matsuda, J. 66 Matsuo, T. 3 Matsuzawa, Y. 3 McCaleb, M.L. 218 McCann, R.A. 220 McClearn, G.E. 164 McConnell, I. 195 McCracken, K.J. 246 McCune, S.A. 287 McGarry, J.D. 45 McInnes, R.R. 56 McIntosh, G.H. 76 McKinley, D.R. 194 McMurray, D.N. 307 McNamara, P.D. 217 Medina, C.A. 191 Meingassner, J.G. 304 Melton, D.W. 321 Mendis, S. 133 Menzies, B.E. 289 Menzies, C. 81 Mercer, L.P. 329 Meredith, D.M. 298 Mertz, R.J. 89 Messina, M.J. 291 Metz, J. 75 Mhaskar, Y. 94 Michaelis, O.E. IV 119, 277 Michalak, A. 263 Mikami, T. 238 Miller, J.F. 54 Miller, K. 216 Miller, P.E. 61 Miller, T.E. 255 Mitchel, R.E.J. 220 Mitkova, A. 131 Mitsumori, K. 266 Miura, K. 168 Miyoshi, I. 134 Moazed, T.C. 300 Montgomery, C. Jr 184 Moon, H.W. 148 Moore, T.B. 198 Morel, F. 225 Moretto, A. 71 Morgan, J.H. 254 Morgane, P.J. 261 Morrison, D.P. 220 Moshe, S. 183 Mote, C.R. 15 Moughan, P.J. 257 Mozrzymas, J.W. 137 Muggenburg, B.A. 7 Muller, P.K. 160 Mulvin, D. 69 Murnane, R.D. 249 Murphy, J.W. 220 Murray, D.L. 314 Murray, P.K. 171 Mutwiri, G.K. 147 Myers, Laurie A. 47 Nagatani, M. 168 Nagy, J.I. 67 Nakagwa, M. 66 Nakayama, M. 85 Narama, I. 68, 168 Nardini, M. 118 Nashold, B.S. Jr 151 National Association for Biomedical Research (U.S.) 322 Nederlandse Centrale Organisatie voor Toegepast- Natuurwetenschappelijk Onderzoek 18 Neef, N.A. 254 Nelson, L.M. 1 Nestor, K.E. 64 Neuringer, M. 141 Newby, F.D. 227 Nicklin, S. 216 Nicolson, L. 298 Nieuwland, M.G.B. 114 Niewiesk, Stefan 253 Nirtles, M.J. 257 Nishikawa, T. 68 Nishimura, M. 68 Niu, C. 160 Nixon, B. 325 Nonneman, Arthur J. 308 Nose, M. 237 Notbohm, H. 160 Nozaki, Y. 238 O'Connor, D.L. 203 Odaka, H. 3 Odle, J. 169 Oehme, F.W. 115 Ogawa, N. 155 Ogilvie, G.K. 9 Ogura, A. 66 Ohneda, M. 45 Ohyama, H. 126 Oki, Y. 189 Okuyama, H. 224 Okwueze, M.I. 41 Olmsted, R.A. 236 Olson, N.C. 305 Olsvik, O. 190 Opgenorth, T.J. 41 Orthen-Gambill, N. 109 Osanai, T. 134 Osborne, M.T. 120 Ostenson, C.G. 192 Osweiler, G. 159 Otis, E.J. 176 Ouding, R.J. 142 Ovelmen-Levitt, J. 151 Ozaki, K. 68 Pace, M.J. 53 Pahud, J.J. 83 Panneton, W.M. 233 Paoletti, S. 137 Papageorges, M. 267 Pasini, E. 250 Paulson, D.J. 57 Pedraza, M. 257 Pelegrin, M. 310 Pena, L. 303 Penicaud, L. 91 Penn, D. 59 Percy, D.H. 293 Persky, V. 291 Peters, C.J. 63 Phalen, S.W. 307 Philbrick, D.J. 127 Philipson, L.H. 89 Phillips, T.J. 162 Phillips, T.R. 236 Picciano, M.F. 203 Pieber, T.R. 112 Pinard, M.H. 114 Pisters, P.W.T. 13 Podbielski, F.J. 133 Pollesello, P. 137 Potgieter, L.N.D. 15 Powell, A.M. 277 Powell, N. 42 Prescott, M.F. 295 Price, R.E. 174 Prieur, D.J. 249 Probert, W.S. 264 Pronczuk, A. \u Brandeis University, Waltham, MA 106 Prospero-Garcia, O. 236 Puaoi, D.L. 236 Pujol, A. 310 Pullen, L.A. 171, 298 Purewal, M. 325 Qian, C.G. 63 Qureshi, I.A. 263 Racz, Paul 32 Radcliffe, J.D. 80 Randall, J.C. 198 Raper, S.E. 194 Rapp-Gabrielson, V.J. 78 Rasmussen, M.A. 37 Ratnakumari, L. 263 Rea, C.T. 217 Recant, L. 119, 277 Reddy, B.S. 99, 102 Rehg, J.E. 125 Reider, E. 166 Reisbick, S. 141 Renegar, K.B. 197 Revilla, Y. 303 Reznik, Gerd 40 Richardson, R.J. 198 Rives, L. 107 Robbins, F.L. 167 Roberts, C.W. 297 Robins, E.D. 1 Robinson, D.R. 296 Roe, M.W. 89 Roebuck, B.D. 101 Rogers, A.E. 110 Rohrbach, M.S. 256 Roitelman, J. 112 Rojkind, M. \u Albert Einstein College of Medicine, Bronx, NY 34 Romeo, J.P. 233 Roos, M.A. 203 Rose, D.P. 104, 268 Rosenberg, L. 312 Rosendal, S. 147 Rosenkrantz, W.S. 74 Rosenthal, H.A. 311 Rosenthal, S. 311 Ross, A.C. 328 Rossi, R.P. 69 Rossitch, E. Jr 151 Rothuizen, J. 259 Rowe, L.C. 255 Rowsell, H.C. 20 Roy, C.C. 202 Rubin, E.M. 39 Rubin, S.A. 49 Runciman, W.B. 14 Russell, J.C. 207, 208, 270 Ruzzier, F. 137 Sachan, D.S. 58 Saegusa, T. 168 Sahin, G. 159 Saint Paul, N. 225 Saito, T. 237 Samuel, J.E. 148 Sanchez, M.S. 135 Sandaradura, S. 72 Sande, R.D. 267 Sanders, T.A.B. 72 Sasaki, M. 189 Sato, M. 180 Satterfield, W. 174 Saudek, C.D. 251 Savoldi, F. 301 Scaccini, C. 118 Scanlon, P.D. 256 Scapellato, M.L. 71 Scelsi, R. 301 Schamber, G.J. 78 Schellekens, H. 21 Schellekens, Huub 18 Scheynius, A. 199 Schmidt-Sommerfeld, E. 59 Schroeder, M.A. 256 Schuller, Hildegard M. 40 Schutz, M.M. 163 Schwan, A. 199 Schwarz, K. 83 Sebokova, E. 131 Segal, S. 217 Seino, Y. 211 Setchell, K.D.R. 291 Shafrir, E. 183 Shamoto, M. 238 Sheikhnejad, G. 222 Shelton, M. 81 Shepherd, P.R. 5 Shimazu, N. 306 Shiraishi, N. 117 Shively, C.A. 26, 128 Shock, Nathan Wetherill, 260 Shrago, E. 130 Shuster, D.E. 185 Silcock, Sheila 319 Simopoulos, A.P. 247 Sklan, D. 193 Smith, C.P. 29, 30, 31 Smith, D.J. 39 Smith, G.P. 33 Smith, J.C. 269 Smith, J.F. 42 Smith, M.O. 58 Smith, W.C. 257 Smyth, J.R. Jr 290 Snoswell, A.M. 14 Soares, J.H. Jr 120 Soltysiak-Pawluczuk, D. 325 Spencer, B. 89 Spennetta, T. 130 Spiegelman, B.M. 314 Spycher, M.A. 157 Sredy, J. 218 Srivastava, R.A.K. 283 Stamp-Cole, M. 142 Standaert, M.L. 200 Starc, T. 137 Stein, D.T. 112 Stephens, L.C. 174 Stevenson, Donald E. 230 Stills, H.F. Jr 287 Stinson, Sherman F.,_1946- 40 Stokes, A. 171, 298 Stokes, C.R. 149 Storb, R. 55 Storts, R.W. 81 Stramm, L. 176 Strandberg, J.D. 251 Stratford-Perricaudet, L.D. 194 Stratum, P. van 124 Strobel, S. 158 Stump, K.C. 251 Su, E.N. 79 Sugano, Michihiro,_1933- 108 Sullivan, M.P. 167 Sundberg, John P. 172 Superti-Furga, A. 157 Suzuki, S. 200 Svec, P. 131 Swanson, J. 28 Swanson, J.C. 27 Swindle, M. Michael 150 Swindle, M.M. 251 Tagaya, O. 238 Taguchi, T. 117 Tahiliani, A.G. 57 Takahashi, H. 127 Takano, K 66 Tanaka, S. 180 Taniguchi, T. 180 Tarui, S. 3 Tashijan, R.J. 140 Tephly, T.R. 159 Thibault, L. 202 Thienpont, E. 50 Thomas, E.D. 55 Thomas, J. A._1933- 47 Thorner, P.S. 56 Thurston, J.R. 272 Timmers, K.I. 277 Todd, J. 186 Todhunter, R.J. 258 Tokunaga, K. 3 Tomassi, G. 118 Tomita, T. 237 Tonkiss, J. 261 Torres-Anjel, M.J. 223 Toyota, T. 200 Tozzo, E. 5 Trott, D.J. 254 Trpis, M. 6 Tshikuka, J.G. 223 Tsuchitani, M. 168 Tsuji, S. 196 Turley, S.D. 271 Uelmen, P.J. 294 Unger, R.H. 45 University of Washington, Primate Information Center 288 Usui, T. 189 Vail, D.M. 9 Vaishnav, S. 184 Valera, A. 310 Van Wyk, C.W. 143 VandeWoude, S.J. 280 Vari, R.C. 41 Venkatraman, J.T. 281 Verschuren, P.M. 124 Vinik, A.I. 312 Vinuela, E. 303 Virmani, K. 179 Vittur, F. 137 Vles, R.O. 124 Vogler, G.A. 233 Volz-Lingenhol, A. 225 Von Bernuth, R.D. 15 Von Geldern, T.W. 41 Voyles, N.R. 119, 277 Vrana, A. 131 Waggie, K.S. 213 Wainfan, E. 222 Wakabayashi, T. 85, 126 Wakamiya, M. 184 Wakasugi, N. 237 Walker, B.E. 239 Walker, M.A. 81 Walker-Smith, J.A. 161 Waltrip, R.W. II 49 Walzem, R.L. 43 Wang, Y. 204 Wang, Y.M. 325 Wang, Z. 200 Warden, C.H. 53 Wargovich, M.J. 174 Warren, J.W. 232 Wasteson, Y. 190 Watanabe, K. 155 Watson, B.J. 233 Watson, R.R. 204 Wattleton, T. 107 Weide, L.G. 177 Weigel, K.A. 272 Weingand, K.W. 26 Weingard, K.W. 226 Weir, V.A. 81 Weise, D. 111 Welch, B.G. 292 West, C. E. 316 West, C.E. 65 Wheeler, S.L. 9 Wheldon, L.A. 298 Whipp, S.C. 37 Whittaker, G.R. 298 Widhalm, K. 179 Wiesmann, U. 157 Wilkins, S.D. 277 Willems, L. 50 Williams, A. 107 Williams, S.C.R. 195 Willis, L.V. 42 Wilson, J.M. 194 Wissler, R.W. 133 Wolf, E. 160 Wolfe, G.L. 244 Wong, M.L. 4 Woodruff, Michael L. 308 Woods, P.R. 81 Worley, J.F. III 89 Wu, Bing-quan,_1930- 187 Wu, X. 184 Wu-Owens, J. 213 Wynder, E.L. 268 Yager, J. 147 Yamada, K. 200 Yamaguchi, T. 127 Yamamoto, T. 211 Yamasaki, K. 86 Yamashita, T. 134 Yamatsu, K. 238 Yamazaki, K. 85, 126 Yan, G. 2 Yancey, R.J. Jr 135 Yang, C. 160 Yang, H. 5 Yang, Y. 200 Yano, H. 211 Yasuda, K. 211 Yen, T.T. 244 Yokomizo, Y. 180 Yoshida, H. 165 Yoshida, M.C. 134 Yoshikawa, Y. 86 Young, E.A. 214 Young, G.P. 105 Young, J.B. 178 Young, J.N. 151 Youson, J.H. \u University of Toronto, Ontario, Canada 46 Yu, D.Y. 79 Zaalberg, J. 124 Zeligman, B.E. 69 Zeller, K.R. 212 Zevenbergen, J.L. 124 Zhang, C. 200 Zheng, Jie 187 Zheng, K. 56 Zicha, Joseph 221 Zijpp, A.J. van der 114 Zucker, I. 284
Abnormal behavior 49 Abnormalities 97 Abortion 186 Abscesses 300 Absorption 257 Acetyl coenzyme a 130 Acetylcholinesterase 71, 115, 198 Acquired immune deficiency syndrome 17, 113, 204, 223, 282 Active transport 5, 314 Activity 155 Acute infections 67 Adenine 116 Adenoviridae 194 Adhesion 324 Adipocytes 5, 200, 227, 314 Adipose tissue 5, 91, 109, 227 Adrenalectomy 252 Adults 191 Adverse effects 258 Aedes mediovittatus 6 African swine fever virus 303 Age 117, 152 Age differences 7, 94, 177 Aging 7, 85, 112, 227, 260 AIDS (Disease) 18, 288 Alcoholism 8, 34, 44, 73, 162 Alleles 2, 294 Allergens 83 Aluminum 164 Alzheimer's disease 52, 164 Amino acid metabolism 13, 318 Amino acid sequences 56 Amino acids 12, 179 Angiotensin 107 Animal behavior 224, 284 Animal breeding 92, 181 Animal diseases 28, 31 Animal experimentation 322 Animal experiments 21, 33, 38, 44, 95, 144, 162, 216, 228, 233, 235, 246, 278 Animal fat 76 Animal health 233, 272 Animal husbandry 233 Animal models 1, 2, 6, 7, 9, 10, 11, 12, 15, 16, 25, 26, 29, 30, 34, 35, 36, 37, 38, 39, 40, 43, 44, 45, 46, 49, 51, 52, 53, 54, 56, 57, 58, 61, 62, 63, 65, 67, 68, 69, 70, 73, 75, 76, 77, 79, 81, 82, 85, 87, 87, 91, 92, 93, 94, 95, 98, 99, 100, 101, 104, 106, 107, 109, 111, 112, 114, 115, 116, 119, 123, 126, 130, 131, 135, 136, 139, 141, 142, 143, 145, 146, 148, 149, 150, 151, 152, 153, 154, 155, 157, 161, 162, 163, 164, 167, 168, 170, 173, 174, 176, 178, 179, 180, 183, 184, 185, 186, 187, 187, 188, 189, 191, 192, 194, 195, 196, 197, 200, 201, 205, 207, 208, 209, 210, 212, 214, 217, 218, 219, 220, 221, 222, 224, 227, 228, 229, 230, 231, 232, 234, 237, 238, 240, 242, 243, 244, 248, 249, 254, 257, 258, 259, 261, 262, 265, 266, 267, 268, 269, 274, 277, 285, 287, 289, 290, 292, 294, 297, 298, 300, 302, 303, 305, 306, 307, 312, 313, 315, 316, 317, 318, 320, 326, 327, 328, 329, 330 Animal models in research 19, 319, 322 Animal nutrition 316 Animal physiology 224 Animal protein 76 Animal proteins 5, 205 Animal research 21 Animal testing alternatives 10, 11 Animal welfare 27, 87, 322 Animals 23, 27, 28, 321 Anorexia 4, 215 Anorexia nervosa 33, 155 Antagonism 317 Antagonists 41 Antibacterial properties 264 Antibiotics 113, 135, 255 Antibodies 158, 206 Antibody formation 49, 114, 186, 264, 328 Antifungal properties 113 Antigens 158, 161, 328 Antimicrobial properties 113 Antioxidants 118, 204, 276, 285 Aphthovirus 166 Apolipoproteins 3, 39, 210, 283, 294 Appetite 24 Application methods 78 Arochlor 144 Arprinocid 125 Arteries 86 Arthritis 87, 137, 267 Ascorbic acid 324, 327 Assays 272 Assessment 296 Atherogenic diet 26, 167 Atherosclerosis 39, 82, 108, 208, 226, 295 Atlases 40, 40, 40, 40 Atresia 46 Attenuation 42 Attractants 275 Autoantibodies 290 Autoimmune diseases 2, 62, 95, 181, 240, 247, 281, 290, 304 Autoimmunity 2, 62, 158 Azoxymethane 174 B lymphocytes 191 Bacteria 199 Bacterial antigens 190 Bacterial count 135 Bacterial diseases 21, 232, 305 Bacterial proteins 54 Bacteroids 254 Beta-galactosidase 194 Beta-glucuronidase 157 Bibliographies 27, 28, 29, 30, 31 Bibliography 274, 274, 274 Bile 320 Bile ducts 46 Bile pigments 170 Biliary calculi 320 Bilirubin 153, 154, 170 Binding 294 Bioavailability 12 Biochemistry 75 Biological rhythms 329 Biological techniques 271 Biotechnology 47, 318 Bladder 232 Blastomere 48 Blood 303 Blood cholesterol 108 Blood coagulation 20 Blood composition 106 Blood flow 20 Blood glucose 251 Blood lipids 1, 45, 118, 133, 282 Blood picture 52 Blood plasma 3, 63, 72, 82, 106, 112, 115, 118, 130, 141, 271, 278 Blood pressure 86, 107, 131, 326 Blood proteins 108 Blood serum 7, 9, 122, 152, 206, 278, 286, 320 Blood sugar 9, 16, 79, 95 Blood vessels 324 Bo RNAdisease virus 49 Body fat 5, 128, 227 Body weight 64, 107, 130, 155, 227 Bone density 120 Bone diseases 160 Bone fractures 273 Bone marrow 191 Bone marrow transplant 55 Bone strength 129, 160 Bordetella bronchiseptica 54 Borrelia burgdorferi 264 Bovine leukosis 185 Bovine mastitis 23, 146, 163, 272 Bovine oncovirus 50, 51, 311 Brain 52, 63, 71, 81, 198, 236, 252, 261 Brain disorders 12 Branched chain amino acids 318 Branhamella 280 Breast feeding 83 Breed differences 163 Breeding value 114, 163 Broilers 58 Brown fat 5 Brugia malayi 6 Brugia pahangi 6 Bulimia nervosa 33 Bulls 185 Cabt 163 Cachexia 9, 13, 147, 215, 282 Calcium 76, 120, 129, 137, 326 Calcium ions 89 Caloric intake 84, 102, 241 Calorie-restricted diets 214 Calories 101 Calves 185 Campylobacter 146 Cancer 187, 230 Candida albicans 143 Candidosis 143 Caprine arthritis encephalitis virus 267 Carbohydrate metabolism 5, 95, 130, 211, 310, 323 Carbohydrate metabolism disorders 9, 109 Carbohydrates 98 Carbon tetrachloride 34, 306 Carcinogenesis 84, 98, 99, 101, 102, 220, 222, 230 Carcinogenicity testing 230 Carcinogens 110, 174, 220 Carcinoma 13, 60, 76, 102, 215, 222, 276, 281, 291, 315, 325 Cardiomyopathy 136, 229 Cardiovascular diseases 57, 228, 281 Carnitine 14, 58, 59 Carotenoids 60, 276 Cartilage 137 Case reports 157, 300 Casein 80, 329 Cat 74 Catabolism 318 Cataract 61 Catecholamines 235 Catheters 232 Cats 43, 90, 149, 157, 176, 236 Cattle 37, 147, 186 Cell culture 166 Cell differentiation 312 Cell growth 312 Cell lines 166 Cell mediated immunity 328 Cell membranes 100 Cell ultrastructure 68 Cells 191 Cellular immunity 62 Central nervous system 52, 224, 236 Cerebral cortex 151 Cerebrospinal fluid 63, 236 Ceroid 81 Characterization 262 Chediak-higashi syndrome 68 Chicken housing 181 Chicks 173, 193 Child development 12 Children 161 Chimeras 48 Chinchillas 206 Chlorpyrifos 71, 198 Cholecalciferol 120 Cholesterol 1, 72, 82, 86, 93, 106, 122, 133, 144, 167, 271, 278, 283, 295 Cholesterol acyltransferase 3 Cholesterol metabolism 106, 194, 320 Chondrocytes 137 Chronic course 25, 73 Chronic infections 297 Cigarettes 324 Ciprofloxacin 135 Circulatory disorders 305 Cirrhosis 259, 306 Clinical trials 100, 276 Clones 42 Cloxacillin 135 Coconut oil 133 Coffee 72 Collagen 56, 160 Colon 76, 99, 102, 105, 174 Colonization 254 Colonizing ability 54 Colostrum 152 Complementary DNA 194 Complications 287 Composition 127, 164 Computed tomography 81, 128 Computer simulation 228 Congenital infection 297 Congresses 187, 187, 187, 187, 230, 230, 230, 230, 230 Contamination 15 Convulsions 85, 319 Cooking oils 36 Copper 117 Coronary vessels 86 Correlation 130 Costs 272 Cotton 256 Cottonseed protein 80 Cows 43, 219 Cretinism 279 Cricetulus barabensis 16 Cross immunity 123 Cross immunization 123 Cryptosporidium 125 Culling 185 Cycling 107 Cytochrome b 225 Cytokines 204, 215 Cytosine 166 Cytosol 205 Dairy cattle 51 Dairy cows 163, 272 Death 191 Deficiency 194, 222 Deficiency diseases 14, 36, 73, 317 Degeneration 81 Deletions 166, 225 Demyelination 75 Dermatophilus congolensis 123 Diabetes 2, 79, 91, 96, 97, 168, 244, 247, 251, 277, 310 Diabetes mellitus 3, 16, 41, 45, 89, 95, 122, 183, 189, 192, 200, 211, 218, 228, 287, 310, 312, 314 Diagnosis 81, 161, 179, 249 Diarrhea 190, 323 Diet 3, 25, 57, 60, 72, 76, 84, 107, 127, 133, 164, 175, 193, 203, 222, 247, 257, 270, 276, 281, 299, 301 Diet studies 325 Diet treatment 179, 215 Dietary carbohydrate 16, 109, 119, 130 Dietary fat 16, 38, 76, 84, 98, 99, 100, 101, 102, 103, 104, 109, 118, 124, 130, 239, 268, 281, 283, 320 Dietary protein 76, 80, 98, 278, 318, 320 Dietary proteins 241 Diethylstilbestrol 239 Diets 144, 167, 226 Digesta 190 Digestion 257 Digestive tract 161 Digestive tract mucosa 182 Digoxin 229 Diploidy 48 Disease course 86, 136, 180 Disease models 1, 9, 10, 11, 15, 17, 20, 21, 27, 28, 29, 31, 48, 51, 61, 66, 69, 77, 78, 82, 93, 96, 111, 117, 134, 136, 137, 140, 143, 145, 146, 147, 148, 149, 156, 164, 165, 167, 168, 174, 176, 181, 184, 189, 220, 223, 226, 228, 229, 234, 237, 238, 251, 292, 295, 306, 309, 313, 315 Disease prevalence 37, 61 Disease prevention 60, 76, 90, 125, 224, 247, 258, 264, 276, 325 Disease resistance 243, 272 Disease surveys 325 Disease transmission 15, 77 Disease vectors 6 Diseases 19, 22, 30, 40, 150, 221, 224, 230, 248, 274, 322 Distribution 128 Dna hybridization 190 Dna methylation 222 Dna probes 318 Docosenoic acids 141, 247, 296 Dogs 7, 9, 55, 56, 74, 94, 111, 136, 176, 217, 258, 259, 300 Domestic animals 197 Dosage 258 Dosage effects 123, 198 Down's syndrome 48 Dracunculus insignis 292 Drinking behavior 44 Drosophila melanogaster 116 Drosophila subobscura 225 Drug combinations 135 Drug effects 24, 125, 135, 258 Drug therapy 74, 122, 215, 258, 311 Drug toxicity 281 Dry period 135 Dusts 256 Ear diseases 304 Eating patterns 132 Edema 148 Eicosanoids 100, 296 Eicosapentaenoic acid 247, 296 Elderly 191, 281 Elderly nutrition 241 Electrocardiograms 136 Elisa 123, 313 Embryonic stem cells 184 Encephalitis 49, 301 Encephalopathy 259 Endocrine glands 191 Endocrine system 189 Endoplasmic reticulum 89 Endothelium 324 Endotoxins 305, 317 Energy expenditure 252 Energy intake 103, 130 Energy metabolism 137, 178, 215, 263 Enteral feeding 182, 281 Enteritis 147 Enterotoxemia 148 Enterotoxins 190, 262 Enzyme activity 89, 94, 115, 116, 157, 198, 200, 311, 318 Enzyme deficiencies 157, 263 Enzymes 254, 258 Epidemiological surveys 268, 276 Epidemiology 51, 223 Epidermal growth factor 169 Epilepsy 319 Epinephrine 63, 178 Epithelium 74 Equine herpesvirus 201, 298 Equine infectious anemia 140 Equine infectious anemia virus 140 Equine influenzavirus 139 Erythrocytes 94, 115 Escherichia 37 Escherichia coli 37, 148, 190, 262, 323 Essential fatty acids 141, 202 Esterases 71, 115, 198 Estradiol 1 Estrogenic properties 291 Estrogens 196 Estrous cycle 155 Ethanol 25, 58, 110 Evolution 247 Exercise 101, 109, 128 Exons 56 Experimental atherosclerosis 26, 93, 144, 210 Experimental diabetes 45, 89, 183, 200, 310 Experimental diets 91, 141, 329 Experimental infection 6, 146, 147, 197, 231 Experimental infections 49, 67, 135, 139, 292, 323 Experiments 232 Fanconi syndrome 217 Fasting 132, 153, 154 Fat absorption 202 Fat consumption 281 Fat deficiencies 141, 202, 281 Fat metabolism 109 Fatal infections 139, 317 Fatty acids 45, 99, 101, 104, 106, 127, 141, 270, 299 Fatty liver 43, 219 Fatty liver hemorrhagic syndrome 43 Feasibility studies 268 Feces 190 Feed conversion efficiency 109 Feed intake 16, 109 Feedback 252 Feeding behavior 24, 155 Feet 67 Feline immunodeficiency virus 90, 236 Feline oncovirus 223 Female animals 155, 239 Fermentation 323 Ferrets 61, 292 Ferritin 52 Fetal alcohol syndrome 173 Fetus 173, 279 Fiber 76, 102, 105 Filariasis 6 Fimbriae 190 Fish oils 38, 99, 101, 127, 131, 141, 270, 281, 285, 296 Foals 152 Folic acid 8, 73, 159, 203 Food 108 Food allergies 83, 158, 161 Food composition tables 247 Food intake 80, 155 Food intolerance 216 Food restriction 155, 241 Food supplements 131 Foodborne diseases 156, 323 Foreign bodies 232 Formates (salts) 159 Formic acid 159 Fowls 70, 71, 114, 181, 290 Fsh 1 Fulvic acids 160 Furazolidone 229 Ganglia 67 Gangliosidosis 249 Gastric ulcer 155 Gastritis 199 Gastroenteritis 161 Gastrointestinal diseases 37, 182 Gene expression 2, 4, 194, 211, 222, 225, 283, 309, 310 Gene therapy 194 Gene transfer 194, 310 Genes 42, 180, 190, 211, 225, 244 Genetic correlation 163 Genetic defects 185 Genetic disorders 321 Genetic engineering 39, 166, 309, 321 Genetic factors 179 Genetic gain 163 Genetic markers 91 Genetic models 53, 162 Genetic regulation 162, 283 Genetic resistance 163 Genetic trend 114 Genetic variation 50 Genistein 291 Genomes 225, 309 Gerbils 167 Germfree state 143 Glomerular filtration rate 41 Glomerulonephritis 66, 149 Glomerulopathy 237 Glomerulus 238 Glucagon 119 Glucocorticoids 191 Gluconeogenesis 310 Glucose 5, 89, 95, 130, 192, 211, 310, 314 Glucose tolerance 5, 9, 91 Glutathione peroxidase 285 Glycerate 2,3-bis(phosphate) 79 Glycerol-3-phosphate acyltransferase 200 Glycogen 168 Glycogenosis 94 Glycolysis 137 Glycoproteins 42, 171, 298 Glycosaminoglycans 176, 258 Gnotobiotic animals 254 Goats 267 Goiter 36, 279 Golden hamsters 312 Gonadotropins 1 Gram negative bacteria 305 Granules 68 Granuloma 180 Growth 227, 329 Growth factors 104 Growth rate 80, 329 Guinea pigs 63, 78, 167, 255, 256, 265, 269, 301, 307 Haemophilus 78 Haemophilus somnus 186 Hair 172 Hamsters 72, 166, 167, 171, 271, 298, 320, 324 Handbooks, manuals, etc 87, 87 Handling 233 Haplotypes 294 Healing 273 Health risk assessment 47 Heart 57, 86 Heart diseases 175, 207, 247, 287 Heart rate 38, 107 Heat stability 160, 262 Hematology 79 Hematopoiesis 300 Hemodialysis 14 Hemodynamics 41 Hemoglobin 79 Hemolysis 289 Hemorrhage 20, 280 Hens 43, 71, 198 Hepatitis 111, 126, 134, 259 Hereditary diseases 56, 131, 176, 177, 181, 194, 238 Heritability 114, 163 Herpes simplex virus 67 Herpetoviridae 171 High density lipoprotein 39, 133, 283 Histidine 289 Histidinemia 179 Histocompatibility antigens 2 Histology 7, 147 Histopathology 61, 66, 68, 86, 155, 168, 174, 180, 189, 229, 238, 249, 266, 267, 295, 306, 313, 315 HIV infections 32 Holstein-friesian 185 Homologous recombination 184 Hormonal control 200, 314 Hormone receptors 183, 314 Hormones 104, 189 Horses 129, 137, 140, 258, 298 Host specificity 77 Human behavior 52 Human diseases 15, 36, 37, 51, 55, 165, 209 Human immunodeficiency virus 17, 204, 223 Human milk 158, 169, 257 Human nutrition research 33, 65, 131, 235, 250, 261, 325, 327 Humoral immunity 328 Hydrolases 285 Hyperbilirubinemia 153, 154, 238 Hypercholesteremia 108 Hypercholesterolemia 1, 106, 122, 194, 278, 294, 295 Hyperglycemia 45, 218, 310 Hyperinsulinemia 16, 130, 183, 226, 299 Hyperlipemia 1, 86, 93, 167, 194 Hyperphenylalaninemia 12 Hyperplasia 5 Hypersensitivity 83 Hypertension 107, 247, 326 Hyperthermia 220 Hypertriglyceridemia 131, 270, 282 Hyperuricemia 184 Hypoglycemia 132 Hypoplasia 259 Hypothalamic lesions 91 Hypothalamus 1, 4 Hypothyroidism 279 Identification 185 Iga 206 Igg 152, 206 Igm 206 Immune competence 272 Immune response 42, 83, 158, 193, 197, 201, 204, 242, 281, 296, 317, 327 Immune serum 206 Immunity 100 Immunization 264, 328 Immunodiagnosis 190, 313 Immunohistochemistry 189 Immunological deficiency 147, 313 Immunological deficiency syndromes 187, 188 Immunological diseases 74 Immunological factors 63, 282 Immunology 187, 187, 188, 242, 301, 327 Immunopathology 49, 191 Immunosuppression 125 Immunosuppressive agents 74 In vitro 198, 272, 289 In vivo 21 Inactivation 275 Inbred strains 143 Incidence 64, 95, 124, 177, 185 Induced mutations 39 Induced resistance 143 Infant development 281 Infant formulas 121 Infant nutrition 243 Infants 257 Infection 15, 90, 156, 303 Infections 161, 282, 293, 328 Infectious diseases 243, 317 Infectivity 166 Inflammation 49, 247, 267, 296 Influenza 197 Influenzavirus 197 Inhibition 115, 198, 258 Inoculation 199 Inoculum 156 Inoculum density 156 Inositol phosphates 200 Insulin 3, 9, 16, 91, 95, 112, 119, 130, 169, 183, 200, 211, 226, 251, 299, 314 Insulin secretion 16, 45, 89, 192 Insulin-like growth factor 169 Intake 106 Interactions 24 Interferon 21, 282 Interleukins 282, 296 Intestinal absorption 3, 121, 161, 202, 271 Intestinal microorganisms 254 Intestinal mucosa 158 Intramuscular injection 255 Intraperitoneal injection 78 Intravenous injection 149 Iodine 36, 279 Ion transport 137 Iron 52, 203, 235 Irrigation 15 Isoenzymes 94 Isolation 206 Isotope labeling 271 Isotypes 206 Japanese quails 64 Joints (animal) 267 Karyotypes 48 Kidney diseases 127, 212 Kidneys 41, 56, 86, 127, 168, 177, 217 Kinetics 13, 198 Laboratory animals 20, 28, 44, 65, 162, 241, 284, 320 Lactation 84, 129, 135, 203 Lactic acid 9 Lampreys 46 Latent infections 67, 148 Lawns and turf 15 Laying performance 64 Lentivirinae 77 Lesions 151, 236 Lethal dose 198 Leukemia 51 Leukocytes 115, 324 Leukotrienes 296 Lh 1 Life cycle 46 Ligaments 64 Line differences 64, 114 Linoleic acid 84, 106, 224 Linolenic acid 224 Lipid metabolism 43, 130, 205, 219, 282 Lipid metabolism disorders 45 Lipid peroxidation 118 Lipids 91, 93, 186, 295 Lipogenesis 205 Lipolysis 299 Lipoproteins 3, 202, 286, 295 Lipotropic factors 222 Lipoxygenase 100 Liquid diets 25 Listeria monocytogenes 156 Literature reviews 8, 16, 38, 39, 43, 46, 51, 52, 57, 65, 73, 75, 77, 84, 90, 91, 95, 98, 100, 102, 103, 109, 158, 161, 163, 169, 178, 179, 182, 191, 197, 204, 212, 215, 219, 223, 243, 244, 247, 250, 252, 257, 258, 259, 261, 268, 276, 278, 281, 282, 290, 291, 296, 305, 317, 326, 328 Litter size 286 Live vaccines 42, 123 Liver 8, 25, 46, 130, 174, 176, 180, 183, 205, 211, 219, 230, 299, 310 Liver cells 194, 310, 318 Liver diseases 34, 46, 170 Livestock 36, 77 Loci 244 Long chain fatty acids 219 Long term experiments 232 Louisiana 136 Low density lipoprotein 1, 39, 118, 133, 194, 278, 294 Lungs 69, 88 Lymph nodes 303 Lymphadenitis 23 Lymphocyte transformation 135 Lymphocyte transformation tests 313 Lymphocytes 100, 330 Lymphoma 9, 74, 213 Lysine 160 Lysosomes 165, 249 Macaca fascicularis 156, 280 Macaca mulatta 141 Magnetic separation 190 Maize oil 133 Major histocompatibility complex 2 Malabsorption 73 Malaria 285 Male animals 227 Males 128 Malnutrition 12, 73, 182, 243, 317 Mammary gland neoplasms 84, 103, 110, 124, 268 Mammary glands 146 Man 12, 37, 43, 57, 71, 77, 197, 212, 278 Mares 152 Markers 304 Mastitis 135 Maternal antibodies 152 Maternal effects 97, 179 Maternal immunity 152 Maternal nutrition 129, 132, 279 Maturation 239 Measurement 112, 265, 271 Medical anthropology 248 Medical research 10, 11, 228, 233 Medical treatment 152 Medicine 322 Melanins 290 Melanoma 142, 315 Membranes 195, 217 Men 13, 133 Menopause 103 Mental ability 52 Mental stress 128 Meriones unguiculatus 106 Messenger RNA 211, 225 Metabolic disorders 116, 244, 263 Metabolic inhibitors 299 Metabolic studies 214 Metabolism 58, 73, 91, 116, 132, 159, 179, 203, 218, 247 Metabolites 116, 120, 195, 198 Methanol 159 Methionine 329 Methodology 221, 221 Methylation 75 Mice 2, 5, 39, 48, 49, 53, 66, 85, 89, 117, 124, 127, 135, 139, 142, 146, 147, 164, 166, 172, 177, 180, 184, 186, 187, 195, 196, 201, 210, 213, 220, 224, 230, 231, 232, 234, 237, 240, 244, 255, 263, 264, 273, 285, 286, 289, 293, 297, 302, 303, 309, 310, 314, 320, 327, 330 Mice as laboratory animals 172 Microtus arvalis 189 Milk 206, 257 Milk production 272 Milk yield 163 Mineral content 52 Mineral deficiencies 52, 160, 175, 191, 235, 279, 301, 317 Mineral metabolism 164, 235 Mineral nutrition 269 Mineral supplements 120 Minerals 241 Miniature pigs 174 Mitochondrial DNA 225 Mitochondrial genetics 225 Mitogens 296 Models 14, 23, 24, 33, 55, 83, 97, 171, 199, 311, 321 Molecular biology 51 Molecular genetics 210 Monitoring 69 Monkeys 82, 128 Monoclonal antibodies 171, 298, 303 Monodelphis domestica 315 Monoenoic fatty acids 281 Morbidity 78, 212 Morphology 227, 292 Mortality 78, 155, 212, 251 Mucopolysaccharidosis 157, 176 Multiple genes 53 Multiple sclerosis 52 Muscle contraction 38 Muscles 183 Muscular hypertrophy 229 Muskrats 233 Mutagenesis 289 Mutants 42, 54, 66, 184, 237, 238, 293, 323 Mutations 42, 50, 56, 185, 244, 290 Mycobacterium bovis 313 Mycobacterium paratuberculosis 147, 180, 234, 302 Mycoses 231 Myocardial ischemia 250 Myristic acid 106 N-nitrosodimethylamine 111 Nadh dehydrogenase 225 Natural killer cells 100, 328 Necrosis 234 Neonatal development 169 Neonates 59, 121, 132, 158, 243, 286 Neoplasms 10, 11, 64, 69, 70, 80, 99, 100, 101, 104, 105, 174, 239, 247, 309, 315 Nephritis 56 Nephropathy 184 Nephrosis 177 Nephrotic syndrome 66 Nervous system 308 Nervous system diseases 71, 115, 139, 145, 151, 198, 204, 266 Neuroleptics 52 Neurons 81, 249, 266 Neuropeptides 4 Neurophysiology 235, 261 Neurosecretory systems 235 Neurotoxicology 308 Neurotoxins 71, 266 Neurotransmitters 12, 52, 252 Neutrophils 135, 204, 243 Newborn animals 269 Nitrogen 86 Nitrogen balance 13 Nitrous oxide 75 Norepinephrine 63, 178 Normal values 79 Norway 190 Nose 280 Nuclear magnetic resonance spectroscopy 195 Nucleotide sequences 50, 56, 185 Nutrient balance 8, 252 Nutrient deficiencies 59, 242, 247, 285 Nutrient intake 103, 128, 129, 241, 268 Nutrient nutrient interactions 76 Nutrient requirements 65, 182 Nutrient sources 247 Nutrient transport 95, 202, 217 Nutrient uptake 217 Nutrition 24, 153, 224 Nutrition physiology 8, 52, 65, 178, 191, 214, 242, 246, 247, 252, 281, 326 Nutrition research 191 Nutritional assessment 182 Nutritional disorders 33 Nutritional intervention 102, 268, 281 Nutritional state 191, 204, 242 Nutritionally induced diseases 316 Nutritive ratio 109 Obesity 3, 45, 53, 57, 91, 92, 95, 104, 107, 109, 112, 119, 132, 178, 205, 211, 218, 227, 244, 245, 246, 252, 270, 277, 287, 299 Olive oil 118 Oncovirinae 77 Opportunistic infections 113, 143 Oral administration 115, 148, 158, 255 Oral contraceptives 82 Organophosphorus compounds 115, 266 Osteoarthritis 248, 258 Osteoporosis 120 Ovariectomy 120 Ovaries 1 Overfeeding 183, 286 Oviducts 64 Oxidation 204, 299 Oxidoreductases 184, 263, 318 Oxygen 250 Pain 296 Palmitic acid 106 Pancreas 16, 101 Pancreas islets 45, 89, 95, 189, 312 Pancreatectomy 251 Papillomas 315 Papio 25 Paralysis 292 Parasite migration 292 Parasites 21 Parenteral feeding 182, 281 Parkinson's disease 52 Pathogenesis 23, 26, 42, 43, 45, 77, 112, 147 Pathogenicity 37, 139, 254, 323 Pathogens 280, 317, 323 Pathology 165, 304 Pathology, Experimental 221 Peptides 41, 169, 234 Perilla 224 Phagocytes 191 Pharmacokinetics 71, 255 Phenotypes 42, 53, 54, 114, 244, 254 Phosphatidylcholines 93 Phosphatidylinositols 200 Phosphoenolpyruvate carboxykinase 310 Phosphofructokinase 94 Phospholipids 86, 141 Phosphorus 137 Phosphorylation 314 Physical activity 4 Physiology 274 Physiology, Experimental 221 Physiopathology 36, 63, 73, 218, 305 Phytate 121 Pichinde virus 63, 265 Pigeons 26, 144 Piglets 190, 257 Pigs 15, 26, 115, 148, 159, 175, 199, 203, 226, 251, 254, 262, 294, 295, 305 Pituitary 1 Pituitary hormones 16 Pituitary-gonadal axis 1 Plant extracts 113 Plant oils 224 Plasma membranes 5 Platelets 296 Polychlorinated biphenyls 144 Polydipsia 141 Polyenoic fatty acids 38, 247, 281 Polygenic inheritance 290 Polypeptides 112 Porcine enterovirus 15 Portal vein 259 Postmortem examinations 81 Postpartum period 129 Potassium 137 Poults 229 Pregnancy 84, 97, 129, 132, 203, 269, 297 Prenatal period 239, 261 Primates 26, 248, 288, 320 Progesterone 1 Proline 160 Promoters 194, 220 Propranolol 229 Prostate 7, 104 Protection 324 Protein deficiencies 261 Protein energy malnutrition 191 Protein intake 212 Protein kinase 183 Protein metabolism 12, 215 Protein secretion 212 Protein synthesis 12 Proteins 195, 285 Proteinuria 237 Protozoal infections 21 Psammomys obesus 183 Puerperium 261 Purification 262 Pyridoxine 326, 327 Pyrophosphatases 89 Qinghaosu 285 Quails 120 Quarantine 233 Rabbits 1, 26, 59, 93, 122, 123, 194, 206, 255, 323 Rabies virus 223 Radiography 69 Radioimmunoassay 112 Ratios 271 Rats 3, 4, 16, 25, 36, 40, 41, 45, 57, 67, 68, 69, 76, 79, 80, 86, 91, 92, 96, 101, 107, 109, 110, 112, 118, 119, 120, 121, 125, 126, 130, 131, 132, 134, 143, 145, 151, 155, 165, 168, 170, 187, 191, 193, 200, 205, 207, 208, 211, 218, 222, 224, 227, 238, 243, 250, 255, 262, 266, 270, 277, 287, 299, 304, 306, 318, 325, 329 Rats as laboratory animals 40 Receptors 1, 41, 194, 294 Recessive genes 237 Recombinant DNA 194 Recombination 166 Recordings 136 Red deer 313 Regeneration 312 Regression analysis 106, 272 Regulation 158, 200, 252 Relaxin 169 Renal failure 86, 212 Renal function 212 Repetitive DNA 50 Replication 137 Reporter genes 194 Research 113, 284, 291 Resistance 211, 299 Respiration 265 Respiratory diseases 23, 256, 280 Restricted feeding 98 Retinoic acid 328 Retinoids 276 Retinol 193, 327, 328 Retroviridae 35 Retrovirus infections 32 Reviews 99, 101, 104 Rhesus monkeys 121 Rheumatism 87 Rheumatoid arthritis 281, 296 Rhinitis 23 Risk 15, 51, 84, 103, 104, 268, 291 Rna 166 Rodents 188 Rodents as laboratory animals 188 Safflower oil 141, 224 Saimiri boliviensis 153 Saimiri sciureus 154 Salmonella 300 Salmonellosis 300 Sarcoma 315 Saturated fats 130, 283 Schistosomiasis 34 Scintigraphy 267 Scrapie 195 Screening 113, 185, 272 Seasonal behavior 284 Selection criteria 163 Selection differential 114 Selection index 163 Selection methods 181 Selection responses 64, 114 Selenium 160, 175, 285 Serotonin 12, 63 Serotypes 78 Serum albumin 149 Sex 117 Sex differences 82 Sex hormones 134 Sex linkage 56 Sheep 14, 23, 50, 81, 219, 249, 311 Skeletal muscle 130, 211 Skin 172, 220 Skin diseases 153, 315 Skin tests 313 Smoke 324 Smooth muscle 64 Sodium 217 Somatic cell count 163 Sorbitol 323 Source fat 241 Soy milk 121 Soy protein 278 Soybean oil 118 Soybean products 291 Species differences 65, 191, 317 Specific dynamic action 109 Sphingomyelins 93 Spinal cord 292 Spirochaetales 254 Spleen 180, 303 Spread 77 Sri lanka 133 Staphylococcus aureus 135, 289 Starvation 182 Strain differences 49, 50, 54, 78, 96, 146, 164, 180, 275, 317 Streptococcus 275 Stress 82, 107, 155, 204, 250, 300, 313 Structural genes 2, 50, 56, 184, 210, 225 Subcutaneous injection 67, 117, 255 Sulfur 285 Supplements 38, 58, 160, 281, 296 Suramin 311 Surface antigens 264 Surgery 250 Surgery, Experimental 150 Survival 116, 269 Susceptibility 6, 180 Swine 274 Swine as laboratory animals 274 Sympathetic nervous system 178, 252 Symptoms 149, 156, 157, 165, 249 Synergism 317 T lymphocytes 2, 158, 193, 201 Targeted mutagenesis 184 Technetium 267 Temperature 235 Testes 7 Testosterone 7 Thalamus 81 Therapy 321 Thrombosis 20 Thymus gland 191 Thyroid diseases 181 Tissues 52, 141, 164 Tobacco smoking 82, 324 Tongue 143 Tongue lesions 143 Toxemia 305 Toxicity 25, 75, 115, 116, 117, 159, 164, 170, 174, 198, 266, 276, 289 Toxicology 115, 266 Toxins 289 Toxoplasma gondii 297 Toxoplasmosis 297 Trace elements 98, 327 Transcription 225 Transduction 54, 291 Transfection 166 Transfer RNA 225 Transferases 153, 170 Transferrin 52 Transgenic animals 5, 39, 210, 310 Transgenics 321 Transport 43 Treatment 74, 170 Trends 281 Triacylglycerol lipase 165 Triacylglycerols 86, 167, 202, 219, 278 Trichosporon beigelii 231 Triglycerides 133 Triolein 118 Trisomy 48 Trypanosoma cruzi 136 Trypanosomiasis 136 Tuberculosis 307 Tumor necrosis factor 135, 314 Tumors 40, 230 Tumors in animals 40 U.S.A. 162, 163 Ultrastructure 189, 266 Ultraviolet radiation 315 Undernutrition 286 Unsaturated fatty acids 118 Urea 86 Uric acid 184 Urination disorders 196 Vaccination 90, 123, 197 Vaccine development 90 Vaccines 90, 186 Vacuoles 176 Valine 329 Vascular diseases 207, 259 Venezuelan equine encephalitis virus 42 Vertical transmission 297 Very low density lipoprotein 118, 210 Veterans 73 Viral diseases 77, 95 Viral proteins 50 Virulence 42, 54, 78, 139, 166, 323 Vision disorders 141 Vitamin a deficiency 269, 328 Vitamin b12 75 Vitamin d 120, 326 Vitamin deficiencies 8, 75, 193, 317, 326 Vitamin deficiency 250 Vitamin e 76, 126, 204, 250, 285, 325, 326, 327 Vitamin supplements 204, 276 Vitamins 65, 98, 241 Waste water 15 Weight 7, 64, 86 Weight gain 132, 329 Weight reduction 57 Women 13, 103, 268 X chromosome 56 Xanthine dehydrogenase 116 Yersinia pseudotuberculosis 254 Young adults 133 Zinc 121, 191, 301 Zoonoses 51
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http://www.nal.usda.gov/awic/pubs/oldbib/qb9514.htm, April 17, 1998