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大鼠脑内神经肽Y受体Y1和Y2亚型配体结合的阳离子敏感性差异。

Differences in cation sensitivity of ligand binding to Y1 and Y2 subtype of neuropeptide Y receptor of rat brain.

作者信息

Parker M S, Crowley W R, Parker S L

机构信息

Department of Pharmacology, University of Tennessee College of Medicine, Memphis, USA.

出版信息

Eur J Pharmacol. 1996 Dec 27;318(1):193-200. doi: 10.1016/s0014-2999(96)00783-2.

Abstract

The binding of selective ligands to the Y1 subtype of neuropeptide Y receptor in rat brain particulates was promoted by Ca2+ and also stimulated by Sr2+, but reversibly reduced by Ba2+, Mg2+, Mn2+, by the organic polycations neomycin and spermidine, and by chelating agents. The alkali monovalent cations inhibited the Ca(2+)-enabled Y1 subtype binding with some selectivity (Cs+ > or = NH4+ > Li+ > Na+, K+), with half-inhibition between 70-120 mM. The specific Y2 subtype binding was enhanced by all alkaline-earth divalent cations, Mn2+, neomycin and spermidine in the range of 0.1-10 mM, and by alkali cations at up to 100 mM, and also by Na+ salts of the chelators EGTA and EDTA. The large disparity in cation sensitivity indicates substantial differences in the structure of the binding sites of the Y1 and Y2 receptors, predictable from known distinct features of ligand epitopes and of primary structure of the receptors.

摘要

选择性配体与大鼠脑微粒中神经肽Y受体Y1亚型的结合受到Ca2+的促进,也受到Sr2+的刺激,但会被Ba2+、Mg2+、Mn2+、有机聚阳离子新霉素和亚精胺以及螯合剂可逆性降低。碱金属单价阳离子以一定的选择性抑制Ca(2+)促进的Y1亚型结合(Cs+≥NH4+>Li+>Na+,K+),半抑制浓度在70 - 120 mM之间。特定的Y2亚型结合在0.1 - 10 mM范围内受到所有碱土二价阳离子、Mn2+、新霉素和亚精胺的增强,在高达100 mM时受到碱金属阳离子的增强,并且还受到螯合剂EGTA和EDTA的钠盐增强。阳离子敏感性的巨大差异表明Y1和Y2受体结合位点的结构存在实质性差异,这可从已知的配体表位和受体一级结构的不同特征预测出来。

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