Impaired glucose tolerance in mice with a targeted impairment of insulin action in muscle and adipose tissue

被引:108
作者
Lauro, D
Kido, Y
Castle, AL
Zarnowski, MJ
Hayashi, H
Ebina, Y
Hayashi, H
Accili, D [1 ]
机构
[1] NICHHD, Dev Endocrinol Branch, NIH, Bethesda, MD 20892 USA
[2] NIDDKD, Diabet Branch, NIH, Bethesda, MD 20892 USA
[3] Univ Tokushima, Inst Enzyme Res, Tokushima 770, Japan
关键词
D O I
10.1038/3112
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Type 2 diabetes is a complex metabolic disorder characterized by peripheral insulin resistance and impaired beta cell function(1,2) Insulin resistance is inherited as a non-mendelian trait(3). In genetically predisposed individuals, resistance of skeletal muscle and adipose tissue to insulin action precedes the onset of clinical diabetes, and is thought to contribute to hyperglycaemia by leading to impaired beta cell function and increased hepatic glucose production(4,5). It is not clear whether beta cell and liver defects are also genetically determined(2). To test the hypothesis that insulin resistance in muscle and fat is sufficient to cause type 2 diabetes in the absence of intrinsic beta cell and liver abnormality, we generated transgenic mice that were insulin-resistant in skeletal muscle and adipose tissue. These mice developed all the prodromal features of type 2 diabetes hut, despite the compounded effect of peripheral insulin resistance and a mild impairment of beta cell function, failed to become diabetic. These findings indicate the need for a critical re-examination of the primary site(s) of insulin resistance in diabetes.
引用
收藏
页码:294 / 298
页数:5
相关论文
共 23 条
[11]  
Kahn CR, 1996, ANNU REV MED, V47, P509
[12]   Exocytosis of insulin promotes insulin gene transcription via the insulin receptor PI-3 kinase p70 s6 kinase and CaM kinase pathways [J].
Leibiger, IB ;
Leibiger, B ;
Moede, T ;
Berggren, PO .
MOLECULAR CELL, 1998, 1 (06) :933-938
[13]  
NISHIYAMA T, 1994, GENE, V141, P187, DOI 10.1016/0378-1119(94)90569-X
[14]   Non-insulin-dependent diabetes mellitus - A genetically programmed failure of the beta cell to compensate for insulin resistance [J].
Polonsky, KS ;
Sturis, J ;
Bell, GI .
NEW ENGLAND JOURNAL OF MEDICINE, 1996, 334 (12) :777-783
[15]   PATHOPHYSIOLOGY OF INSULIN-RESISTANCE IN HUMAN-DISEASE [J].
REAVEN, GM .
PHYSIOLOGICAL REVIEWS, 1995, 75 (03) :473-486
[16]   INSULIN-RESISTANCE AND GROWTH-RETARDATION IN MICE LACKING INSULIN-RECEPTOR SUBSTRATE-1 [J].
TAMEMOTO, H ;
KADOWAKI, T ;
TOBE, K ;
YAGI, T ;
SAKURA, H ;
HAYAKAWA, T ;
TERAUCHI, Y ;
UEKI, K ;
KABURAGI, Y ;
SATOH, S ;
SEKIHARA, H ;
YOSHIOKA, S ;
HORIKOSHI, H ;
FURUTA, Y ;
IKAWA, Y ;
KASUGA, M ;
YAZAKI, Y ;
AIZAWA, S .
NATURE, 1994, 372 (6502) :182-186
[17]  
TOLMAN EL, 1973, J BIOL CHEM, V248, P4552
[18]   LIPOTOXICITY IN THE PATHOGENESIS OF OBESITY-DEPENDENT NIDDM - GENETIC AND CLINICAL IMPLICATIONS [J].
UNGER, RH .
DIABETES, 1995, 44 (08) :863-870
[19]   Protection from obesity-induced insulin resistance in mice lacking TNF-alpha function [J].
Uysal, KT ;
Wiesbrock, SM ;
Marino, MW ;
Hotamisligil, GS .
NATURE, 1997, 389 (6651) :610-614
[20]   Hyperinsulinemia but no diabetes in transgenic mice homozygously expressing the tyrosine kinase-deficient human insulin receptor [J].
Wang, LH ;
Muromoto, N ;
Hayashi, H ;
Mitani, Y ;
Uehara, H ;
Izumi, K ;
Ebina, Y .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1997, 240 (02) :446-451