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在分离的大鼠脂肪细胞中,氯喹降低了受体介导的胰岛素降解。

Receptor mediated insulin degradation decreased by chloroquine in isolated rat adipocytes.

作者信息

Kobayashi M, Iwasaki M, Shigeta Y

出版信息

J Biochem. 1980 Jul;88(1):39-44.

PMID:6997286
Abstract

The time-course of insulin binding to isolated adipocytes pretreated with chloroquine (0.1 mM) showed that no steady state condition was reached and that the binding kept increasing with the time of incubation up to three hours. Sixty-one percent of the bound labeled insulin could not be dissociated from these cells by 100 microgram/ml of unlabeled insulin, whereas 86% dissociated from the control cells. Chromatography revealed that the bound intact insulin, which had the ability to bind to insulin receptors of adipocytes, was increased and that degraded insulin decreased in the chloroquine treated cells. However, these cells showed normal insulin stimulation of 2-deoxy-glucose uptake. The data suggest that insulin is internalized in adipocytes after binding to insulin receptors and that insulin is degraded at the site, probably lysosomes, where chloroquine inhibits this degradation process.

摘要

胰岛素与用氯喹(0.1 mM)预处理的分离脂肪细胞结合的时间进程表明,未达到稳态,并且结合量随孵育时间增加,直至三小时。100微克/毫升未标记胰岛素不能从这些细胞中解离61%的结合标记胰岛素,而从对照细胞中解离86%。色谱分析显示,氯喹处理的细胞中,具有与脂肪细胞胰岛素受体结合能力的完整结合胰岛素增加,降解胰岛素减少。然而,这些细胞对2-脱氧葡萄糖摄取的胰岛素刺激显示正常。数据表明,胰岛素与胰岛素受体结合后在脂肪细胞内内化,并且胰岛素在氯喹抑制该降解过程的部位(可能是溶酶体)被降解。

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