一种通过寡肽介质形成实现胰岛素作用的蛋白水解机制。
A proteolytic mechanism for the action of insulin via oligopeptide mediator formation.
作者信息
Larner J, Cheng K, Schwartz C, Kikuchi K, Tamura S, Creacy S, Dubler R, Galasko G, Pullin C, Katz M
出版信息
Fed Proc. 1982 Sep;41(11):2724-9.
Evidence is presented that the chemical mediator of insulin action is a peptide(s) and most likely glycopeptide(s). The mediator is formed proteolytically because 1) protease inhibitors inhibit insulin action and 2) trypsin mimicks insulin action via mediator formation. Trypsin mediator does not faithfully reproduce the action of insulin mediator, which indicates that the sites of proteolytic cleavage by insulin and trypsin differ. A coordinated multivalent proteolytic mechanism by which insulin acts to trigger an external membrane-bound protease to cleave mediator from a membrane glycoprotein precursor is presented.
有证据表明,胰岛素作用的化学介质是一种肽或很可能是一种糖肽。该介质是通过蛋白水解形成的,原因如下:1)蛋白酶抑制剂会抑制胰岛素作用;2)胰蛋白酶通过介质形成模拟胰岛素作用。胰蛋白酶介质不能如实地重现胰岛素介质的作用,这表明胰岛素和胰蛋白酶的蛋白水解切割位点不同。本文提出了一种协调的多价蛋白水解机制,胰岛素通过该机制促使一种外部膜结合蛋白酶从膜糖蛋白前体上切割下介质。
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