Approach to the pathogenesis of NIDDM using knockout mouse models.

1999 Fiscal Year Final Research Report Summary

• Project/Area Number: 09470215
• Research Category: Grant-in-Aid for Scientific Research (B)
• Allocation Type: Single-year Grants
• Section: 一般
• Research Field: 内分泌・代謝学
• Research Institution: The University of Tokyo
• Principal Investigator: KADOWAKI Takashi Faculty of Medicine, University of Tokyo, Lecturer, 医学部・附属病院, 講師 (30185889)
• Co-Investigator(Kenkyū-buntansha): YASUDA Kazuki Faculty of Medicine, University of Tokyo, Assistant Medical staff, 医学部・附属病院, 医員 ; TAMEMOTO Hiroyuki Faculty of Medicine, University of Tokyo, Assistant Medical staff, 医学部・附属病院, 医員 ; TOBE Kazuyuki Faculty of Medicine, University of Tokyo, Assistant Medical staff, 医学部・附属病院, 助手 (30251242) ; TERAUCHI Yasuo Faculty of Medicine, University of Tokyo, Lecturer, 医学部・附属病院, 医員
• Project Period (FY): 1997 – 1999
• Keywords: NIDDM / knockout mice / IRS-1 / IRS-2 / insulin resistance / β-cell / glucokinase / NADH shuttle / PI3-kinase

Research Abstract

Non-insulin dependent diabetes mellitus (NIDDM) is caused by interactions of multiple genes and environmental factors. We have been employing knockout mice models to dissect the complex molecular mechanisms of NIDDM. We have generated knockout mice of both IRS-1 and IRS-2, two major substrates for the insulin receptor kinase. IRS-1 knockout mice show skeletal muscle insulin resistance, whereas IRS-2 knockout mice show liver insulin resistance. Despite a similar degree of insulin resistance, IRS-1 knockout mice show compensatory β-cell hyperplasia, whereas IRS-2 knockout mice, show decreased β-cell mass and develop NIDDM. These results suggest that IRS-1 and IRS-2 play distinct roles in skeletal muscle, liver and β-cell, and that both insulin resistance and a defect in.β-cell are required for the development of NIDDM. We have also investigated the role of several genes in theβ-cell functions by targeted disruption of glucokinase (GK) and NADH shuttle system. The results show that glucose metabolism via the classical pathway (TCA cycle) and the NADH shuttle system are both required for glucose-induced insulin secretion. Moreover, IRS-1, IRS-2 and PI3-kinase appear to play regulatory roles inβ-cell functions such as glucose-induced insulin secretion. The development of NIDDM by reconstitution of genetic mutations, each of which alone does not lead to major metabolic alterations, validated the polygenic concept of NIDDM, Interplay between insulin secretory defect and insulin resistance, exemplified byβ-cell bK/IRS-1 double-knockout mice and IRS-2-knockout mice, appears to be a common pathway in the development of NIDDM. Thus, the genetic manipulation of defects in human diabetogenic genes in mice via targeted disruption will provide important insights into the molecular mechanisms and actual biochemical pathways of human NIDDM.

Research Products

• [Publications] Teraichi,Y.,Kadowaki, T., et cl.: "Development of non-insaliu-dependent diabetes mellitus in the double knockout mice with distuption of insulia receptor substrote-land-cell glucokiuqse genes"J. Clin. Invest. 99. 861-866 (1997)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Kaburagi, Y., Kadouaki, T., et al.: "Role of insuliu receptor substrate land pp60 in the regulation of inculin-induced glucose transport and GLUT4 translocation in primary adipocytes"J. Biol. Chem.. 272. 25839-25844 (1997)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Yin, Y., Kadouaki, T., et al.: "Involvement of p85 in p53-dependent apoptotic response to oxidative stress"Nature. 391. 707-701 (1998)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Terauchi, Y., Kadouaki, T. et al.: "Increased insuliu sensitivity and hypoglycemia iu mice lacking p85 subunit of phosphoinositide 3 kinase"Nature Genestics. 21. 230-235 (1999)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Kubota, N, Kadouaki, T., et al.: "PPAEe mediates high-fat diet induced adipocyte hypertrophy and insulin resistance"Mol. Cell. 4. 597-609 (1999)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Terauchi, Y., Kadouaki, T. et al.: "Insulin effect during embryogenesis determiues fetal growth apossible molocular link between birth weight and susceptibility to 2 diable"Diabetes. 40. 82-86 (2000)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Kaburagi, Y., Kadowaki, T, et al: "The mechanism of insulin-induced signal transduction mediated by the insulin receptor substrate family"Endocrine J. 46. 25-34 (1999)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Kadowaki, T., Kubota N., et al.: "Role of PPARr in high-fat diet-induced adipocyte hypertrophy and insulin resistance"Common Disease-Genetic and Pathogenic Aspects of Multifoetorial Disease Uehara Memorial Foudation Symposium-1999. 79-89 (1999)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Terauchi, Y., Iwamoto, K., Tamemoto, H., Komeda, K., Ishii, C., Kanazawa, Y., Asanuma, N., Aizawa. T., Akanuma. Y., Yasuda, K., Kodama, T., Tobe, Y., Yazaki, Y., and Kadowaki, T.: "Development of non-insulin-dependent diabetes mellitus in the double knockout mice with disruption of insulin receptor substrate-1 and β-cell glucokinase genes : genetic reconstitution of diabetes as a polygenic disease."J. Clin. Invest.. 99. 861-866 (1997)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Kaburagi, Y., Satoh, S., Tamemoto, H., Yamamoto-Honda, R., Tobe, K., Ueki, K., Yamauchi, T., Kono-Sugita, E., Sekihara, H., Aizawa, S., Cushman, S. W., Akanuma, Y., Yazaki, Y., and Kadowaki, T.: "Role of insulin receptor substrate-1 and pp60 in the regulation of insulin-induced glucose transport and GLUT4 translocation in primary adipocytes."J. Biol. Chem.. 272. 25839-25844 (1997)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Yin, Y., Terauchi, Y., Solomon, G., Aizawa, S., Yazaki, Y., Kadowaki, T., and Barrett, J. C.: "Involvement of p85 in p53-dependent apoptotic response to oxidative stress."Nature. 391. 707-710 (1998)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Terauchi, Y., Tsuji, Y., Satoh, S., Minoura. H., Murakami, K., Okuno, A., Inukai, K., Asano, T., Kaburagi, Y., Ueki, K., Nakajima, H., Hanafusa T., Matsuzawa, Y., Sekihara, H., Yin, Y., Barrett, J. C., Oda, H., Ishikawa, T., Akanuma, Y., Komuro, I., Suzuki, M., Yamamura, K., Kodama, T., Suzuki, H., Koyasu, S., Aizawa, S., Tobe, K., Fukui, Y., Yazaki. Y., and Kadowaki, T.: "Increased insulin sensitivity and hypoglycemia in mice lacking p85α subunit of phosphoinositide 3-kinase."Nature Genetics. 21. 230-235 (1999)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Kubota, N., Terauchi, Y., Miki, H., Tamemoto, H., Yamauchi, T., Komeda, K., Satoh, S., Nakano, R., Ishii, C., Sugiyama, T., Eto, K., Tsubamoto, Y., Okuno, A., Murakami, K., Sekihara, H., Hasegawa, G., Naito, M., Toyoshima, Y., Tanaka, S., Shiota, K., Kitamura, T., Fujita, T., Ezaki, O., Aizawa, S., Nagai, R., Tobe, K., kimura, S., and Kadowaki, T.: "PPARγ mediates high-fat diet-induced adipocyte hypertrophy and insulin resistance."Mol. Cell. 4. 597-609 (1999)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Terauchi, Y., Kubota, N., Tamemoto, H., Sakura, H., Nagai, R., Akanuma, Y., Kimura, S., and Kadowaki, T.: "Insulin effect curing embryogenesis determines fetal growth. : a possible molocular link between birth weight and susceptibility to type 2 diabetes."Diabetes. 40. 82-86 (2000)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Kaburagi, Y., Yamauchi, T., Yamamoto-Honda, R., Ueki, K., Tobe, K., Akanuma, Y., Yazaki, Y., and Kadowaki, T.: "The mechanism of insulin-induced signal transduction mediated by the insulin receptor substrate family."Endocrine J. 46. 25-34 (1999)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Kadowaki, T., Kubota, N., Terauchi, Y., Miki, H., Tamemoto, H., Yamauchi, T. Komeda, K. Tobe, K., and Kimura, S.: "Role of PPARγ in high-fat diet-induced adipocyte hypertrophy and insulin resistance."Common Disease - Genetic and Pathogenic Aspects of Multifactorial Diseases Uehara Memorial Foundation Symposium- 1999. 79-89 (1999)
  • Description: 「研究成果報告書概要(欧文)」より