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半胱胺可阻断生长抑素分泌,而不改变胰岛素或胰高血糖素的释放过程。一种用于研究胰岛功能的新模型。

Cysteamine blocks somatostatin secretion without altering the course of insulin or glucagon release. A new model for the study of islet function.

作者信息

Sorenson R L, Grouse L H, Elde R P

出版信息

Diabetes. 1983 Apr;32(4):377-9. doi: 10.2337/diab.32.4.377.

Abstract

Cysteamine (300 mg/kg) administered subcutaneously depletes pancreatic somatostatin to 36% of control levels, but does not alter pancreatic insulin or glucagon content. Although perfusion of pancreata from normal animals with glucose (300 mg/dl) markedly stimulated somatostatin release, pancreata from cysteamine-treated animals failed to secrete somatostatin in response to glucose. Cysteamine treatment was without effect on insulin and glucagon release under the conditions tested. The isolated perfused pancreas from the cysteamine-treated rat provides a model for further investigations into regulation of islet hormone release in the absence of stimulated somatostatin release.

摘要

皮下注射半胱胺(300毫克/千克)可使胰腺生长抑素降至对照水平的36%,但不会改变胰腺胰岛素或胰高血糖素的含量。尽管用葡萄糖(300毫克/分升)灌注正常动物的胰腺可显著刺激生长抑素释放,但半胱胺处理动物的胰腺对葡萄糖无生长抑素分泌反应。在测试条件下,半胱胺处理对胰岛素和胰高血糖素的释放没有影响。来自半胱胺处理大鼠的离体灌注胰腺为在无刺激生长抑素释放情况下进一步研究胰岛激素释放的调节提供了一个模型。

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