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加州电鳐膜结合型乙酰胆碱受体中配体诱导的构象变化。

Ligand-induced conformation changes in Torpedo californica membrane-bound acetylcholine receptor.

作者信息

Quast U, Schimerlik M, Lee T, Witzemann T L, Blanchard S, Raftery M A

出版信息

Biochemistry. 1978 Jun 13;17(12):2405-14. doi: 10.1021/bi00605a024.

Abstract

A time-dependent increase in ligand affinity has been studied in cholinergic ligand binding to Torpedocalifornica acetylcholine receptor by inhibition of the kinetics of of [125I]-alpha-bungarotoxin-receptor complex formation. The conversion of the acetylcholine receptor from low to high affinity form was induced by both agonists and antagonists of acetylcholine and was reversible upon removal of the ligand. The slow ligand induced affinity change in vitro resembled electrophysiological desensitization observed at the neuromuscular junction and described by a two-state model (Katz, B., & Thesleff, S. (1957) J. Physiol. 138, 63). A quantitative treatment of the rate and equilibrium constants determined for binding of the agonist carbamoylcholine to membrane bound acetylcholine receptor indicated that the two-state model is not compatible with the in vitro results.

摘要

通过抑制[125I] -α-银环蛇毒素-受体复合物形成的动力学,研究了胆碱能配体与加州电鳐乙酰胆碱受体结合时配体亲和力随时间的增加。乙酰胆碱受体从低亲和力形式向高亲和力形式的转变是由乙酰胆碱的激动剂和拮抗剂诱导的,并且在去除配体后是可逆的。体外缓慢的配体诱导的亲和力变化类似于在神经肌肉接头处观察到的电生理脱敏,并由双态模型描述(Katz, B., & Thesleff, S. (1957) J. Physiol. 138, 63)。对激动剂氨甲酰胆碱与膜结合的乙酰胆碱受体结合所确定的速率和平衡常数的定量处理表明,双态模型与体外结果不相符。

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