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孕期激素在胰岛素抵抗诱导中的作用。

Role of gestational hormones in the induction of insulin resistance.

作者信息

Ryan E A, Enns L

机构信息

Department of Medicine, University of Alberta, Edmonton, Canada.

出版信息

J Clin Endocrinol Metab. 1988 Aug;67(2):341-7. doi: 10.1210/jcem-67-2-341.

Abstract

Pregnancy is associated with insulin resistance. We studied insulin binding and postbinding function in isolated adipocytes from pregnant and nonpregnant rats. We also used a primary culture system for female virgin rat adipocytes to assess the effects of gestational hormones in vitro on insulin binding and postbinding function. Insulin binding to adipocytes was normal during pregnancy, but [14C]3-O-methylglucose transport was reduced. When hCG or estradiol was added to the culture medium, no change in maximum [14C]3-O-methylglucose transport was found; however, maximum insulin binding was increased with estradiol. Progesterone and cortisol both decreased maximum insulin binding and [14C]3-O-methylglucose transport. PRL and placental lactogen decreased maximum [14C]3-O-methylglucose transport, but did not change insulin binding. When these hormones were added concurrently no change in insulin binding was found, but maximum [14C]3-O-methylglucose transport was reduced. We conclude that the insulin resistance of pregnancy is associated with a postbinding defect in insulin action. Estradiol increased insulin receptor binding, but during pregnancy this effect may be offset by the reduction in insulin binding induced by progesterone and cortisol. The postbinding defect in insulin action during pregnancy is probably related to increasing amounts of progesterone, cortisol, PRL, and placental lactogen.

摘要

妊娠与胰岛素抵抗有关。我们研究了妊娠大鼠和未妊娠大鼠分离脂肪细胞中的胰岛素结合及结合后功能。我们还使用了雌性未孕大鼠脂肪细胞的原代培养系统来评估妊娠激素在体外对胰岛素结合及结合后功能的影响。妊娠期间胰岛素与脂肪细胞的结合正常,但[14C]3 - O - 甲基葡萄糖转运减少。当向培养基中添加人绒毛膜促性腺激素(hCG)或雌二醇时,[14C]3 - O - 甲基葡萄糖的最大转运未发现变化;然而,雌二醇会增加胰岛素的最大结合量。孕酮和皮质醇均降低胰岛素的最大结合量以及[14C]3 - O - 甲基葡萄糖的转运。催乳素(PRL)和胎盘催乳素降低[14C]3 - O - 甲基葡萄糖的最大转运,但不改变胰岛素结合。当同时添加这些激素时,胰岛素结合未发现变化,但[14C]3 - O - 甲基葡萄糖的最大转运减少。我们得出结论,妊娠的胰岛素抵抗与胰岛素作用的结合后缺陷有关。雌二醇增加胰岛素受体结合,但在妊娠期间,这种作用可能被孕酮和皮质醇诱导的胰岛素结合减少所抵消。妊娠期间胰岛素作用的结合后缺陷可能与孕酮、皮质醇、催乳素和胎盘催乳素水平的增加有关。

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