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囊泡乙酰胆碱转运体中的一个关键组氨酸。

A critical histidine in the vesicular acetylcholine transporter.

作者信息

Keller J E, Parsons S M

机构信息

Department of Chemistry and The Neuroscience Research Institute, University of California, Santa Barbara, CA 93106, USA.

出版信息

Neurochem Int. 2000 Feb;36(2):113-7. doi: 10.1016/s0197-0186(99)00110-2.

Abstract

The role of proton binding sites in the vesicular acetylcholine transporter was investigated by characterization of the pH dependence for the binding of [3H]vesamicol [(-)-trans-2-(4-phenylpiperidino)cyclohexanol] to Torpedo synaptic vesicles. A single proton binds to a site with pKa 7.1 +/- 0.1, which is characteristic of histidine, to competitively inhibit vesamicol binding. The histidine-selective reagent diethylpyrocarbonate causes time-dependent inhibition of [3H]vesamicol binding with a rate constant only about 20-fold lower than for reaction with free histidine. Because its pH titration has a simple, ideal shape, this residue probably controls all pH effects in the transporter between pH 6-8. Inhibition of [3H]vesamicol binding by diethylpyrocarbonate was slowed by vesamicol but not acetylcholine, which binds to a separate site. The data suggest that a critical histidine with a pKa of 7.1 is unhindered when reacting with diethylpyrocarbonate. A conformational model for the histidine is proposed to explain why acetylcholine competes with protons but not with diethylpyrocarbonate. A conserved histidine in transmembrane helix VIII possibly is the histidine detected here.

摘要

通过对[³H]维西卡米((-)-反式-2-(4-苯基哌啶基)环己醇)与电鳐突触小泡结合的pH依赖性进行表征,研究了质子结合位点在囊泡乙酰胆碱转运体中的作用。一个质子与一个pKa为7.1±0.1的位点结合,该位点具有组氨酸的特征,可竞争性抑制维西卡米的结合。组氨酸选择性试剂焦碳酸二乙酯对[³H]维西卡米结合产生时间依赖性抑制,其速率常数仅比与游离组氨酸反应低约20倍。由于其pH滴定具有简单、理想的形状,该残基可能控制了转运体在pH 6 - 8之间的所有pH效应。焦碳酸二乙酯对[³H]维西卡米结合的抑制作用因维西卡米而减缓,但不受与另一个位点结合的乙酰胆碱的影响。数据表明,一个pKa为7.1的关键组氨酸在与焦碳酸二乙酯反应时不受阻碍。提出了一个组氨酸的构象模型来解释为什么乙酰胆碱与质子竞争但不与焦碳酸二乙酯竞争。跨膜螺旋VIII中一个保守的组氨酸可能就是此处检测到的组氨酸。

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