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胰岛素与人脂肪细胞受体的解离。负协同模型的评估。

Insulin dissociation from its receptors on human fat cells. Evaluation of the negative cooperativity model.

作者信息

Arner P, Bolinder J, Ostman J

出版信息

Acta Diabetol Lat. 1983 Jul-Sep;20(3):197-203. doi: 10.1007/BF02581263.

Abstract

Insulin dissociation from its receptors on isolated human fat cells was investigated using mono-125I-[Tyr A 14]-insulin. Fat cells were equilibrated with 0.05 pmol/ml of the radioligand and then transferred to a radioactive free buffer. The rate of dilution-induced dissociation of bound labelled insulin was enhanced in the presence of native insulin (1.7 nmol/ml), both at 24 degrees C and 37 degrees C and in both omental and subcutaneous adipocytes. The dissociation of radioactive insulin was more rapid when fat cells were equilibrated with 0.15 than with 0.05 pmol/ml of radioactive insulin, both in the presence or absence of an excess of native insulin. Thus, the presence of site-site interactions of the negative cooperativity type among insulin receptors of human fat cells is demonstrated.

摘要

使用单 - 125I - [酪氨酸A14] - 胰岛素研究了胰岛素与分离的人脂肪细胞上受体的解离情况。脂肪细胞用0.05 pmol/ml的放射性配体平衡,然后转移到无放射性的缓冲液中。在天然胰岛素(1.7 nmol/ml)存在下,无论是在24℃还是37℃,以及在网膜和皮下脂肪细胞中,结合的标记胰岛素的稀释诱导解离速率均增强。当脂肪细胞用0.15 pmol/ml而非0.05 pmol/ml的放射性胰岛素平衡时,无论是否存在过量的天然胰岛素,放射性胰岛素的解离都更快。因此,证明了人脂肪细胞胰岛素受体之间存在负协同作用类型的位点 - 位点相互作用。

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