Pete G, Fuller C R, Oldham J M, Smith D R, D'Ercole A J, Kahn C R, Lund P K
Department of Physiology, University of North Carolina, Chapel 27599-7545, USA.
Endocrinology. 1999 Dec;140(12):5478-87. doi: 10.1210/endo.140.12.7219.
Organ weight was compared in adult mice with deletion of one (IRS-1-/+) or both (IRS-1-/-) copies of the insulin receptor substrate-1 (IRS-1) gene and IRS-1+/+ littermates. IRS-1-/+ mice showed modest reductions in weight of most organs in proportion to a decrease in body weight. IRS-1-/- mice showed major reductions in weight of heart, liver, and spleen that were directly proportional to a decrease in body weight. In IRS-1-/- mice, kidney and particularly small intestine and brain exhibited proportionately smaller weight reductions, and gastrocnemius muscle showed a proportionately greater weight reduction than the decrease in body weight. Growth deficits in IRS-1-/- mice could reflect impaired actions of multiple hormones or cytokines that activate IRS-1. To assess the requirement for IRS-1 in insulin-like growth factor I (IGF-I)-dependent postnatal growth, IRS-1-/+ mice were cross-bred with mice that widely overexpress a human IGF-I transgene (IGF+) to generate IGF+ and wild-type mice on an IRS-1+/+, IRS-1-/+, and IRS-1-/- background. IGF-I overexpression increased body weight and weight of brain, small intestine, kidney, spleen, heart, and gastrocnemius muscle in IRS-1+/+ mice. IGF-I overexpression could not completely reverse the body growth retardation in IRS-1-/- mice. Absolute or partial IRS-1 deficiency impaired IGF-I-induced body overgrowth more in females than in males. In males and females, IGF-I stimulated similar overgrowth of brain regardless of IRS-1 status, and intestine and spleen showed dose dependence on IRS-1 for IGF-I-induced growth. IGF-I-induced growth of gastrocnemius muscle had an absolute requirement for IRS-1. IGF-I-induced growth of kidney and heart was impaired by IRS-1 deficiency only in females. In vivo, therefore, most organs do not require IRS-1 for IGF-I-induced growth and can use alternate signaling molecules to mediate IGF-I action. Other organs, such as gastrocnemius muscle, require IRS-1 for IGF-I-induced growth in vivo.
将胰岛素受体底物-1(IRS-1)基因的一个拷贝(IRS-1-/+)或两个拷贝(IRS-1-/-)缺失的成年小鼠与IRS-1+/+同窝小鼠的器官重量进行了比较。IRS-1-/+小鼠大多数器官的重量适度减轻,与体重下降成比例。IRS-1-/-小鼠的心脏、肝脏和脾脏重量大幅减轻,与体重下降直接成比例。在IRS-1-/-小鼠中,肾脏,尤其是小肠和大脑的重量减轻比例较小,而腓肠肌的重量减轻比例大于体重下降比例。IRS-1-/-小鼠的生长缺陷可能反映了多种激活IRS-1的激素或细胞因子的作用受损。为了评估IRS-1在胰岛素样生长因子I(IGF-I)依赖性出生后生长中的需求,将IRS-1-/+小鼠与广泛过表达人IGF-I转基因(IGF+)的小鼠杂交,以在IRS-1+/+、IRS-1-/+和IRS-1-/-背景下产生IGF+和野生型小鼠。IGF-I过表达增加了IRS-1+/+小鼠的体重以及大脑、小肠、肾脏、脾脏、心脏和腓肠肌的重量。IGF-I过表达不能完全逆转IRS-1-/-小鼠的身体生长迟缓。绝对或部分IRS-1缺乏对IGF-I诱导的身体过度生长的损害在雌性中比在雄性中更严重。在雄性和雌性中,无论IRS-1状态如何,IGF-I刺激大脑的过度生长相似,并且小肠和脾脏对IGF-I诱导的生长表现出对IRS-1的剂量依赖性。IGF-I诱导的腓肠肌生长绝对需要IRS-1。IGF-I诱导的肾脏和心脏生长仅在雌性中因IRS-1缺乏而受损。因此,在体内,大多数器官在IGF-I诱导的生长中不需要IRS-1,并且可以使用替代信号分子来介导IGF-I的作用。其他器官,如腓肠肌,在体内IGF-I诱导的生长中需要IRS-1。
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