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首页> 外文期刊>Bioorganic and medicinal chemistry >Structure-affinity relationship studies on arylpiperazine derivatives related to quipazine as serotonin transporter ligands. Molecular basis of the selectivity SERT/5HT(3) receptor.
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Structure-affinity relationship studies on arylpiperazine derivatives related to quipazine as serotonin transporter ligands. Molecular basis of the selectivity SERT/5HT(3) receptor.

机译:结构相关性研究与作为血浆素转运蛋白配体的喹哌嗪有关的芳基哌嗪衍生物。选择性SERT / 5HT(3)受体的分子基础。

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摘要

A series of quipazine derivatives, previously synthesized to probe the 5-HT(3) receptor, was evaluated for its potential interaction with serotonin transporter (SERT). Some of them show nanomolar affinity for the rodent SERT comparable to or slightly higher than quipazine or N-methylquipazine. Subsequently a candidate was selected on the basis of its SERT affinity and submitted to a molecular manipulation of the basic moiety. The structure-affinity relationships obtained provided information on the role of the fused benzene ring of quipazine in the interaction with the SERT binding site and on the stereoelectronic requirements for the interaction of both the heteroaromatic component and the basic moiety. Moreover, the comparison of the structure-affinity relationships obtained in the present work with those concerning the interaction of these heteroarylpiperazine derivatives with 5-HT(3) receptor suggested some molecular determinants of the selectivity SERT/5HT(3) receptor.
机译:评估了一系列先前合成来探测5-HT(3)受体的喹嗪衍生物与5-羟色胺转运蛋白(SERT)的潜在相互作用。它们中的一些显示出对啮齿动物SERT的纳摩尔亲和力与喹嗪或N-甲基喹嗪相当或稍高。随后,根据其SERT亲和力选择候选对象,并对其基本部分进行分子操作。获得的结构亲和性关系提供了有关喹嗪的稠合苯环在与SERT结合位点相互作用中的作用以及对杂芳族组分和基本部分相互作用的立体电子要求的信息。此外,在本工作中获得的结构亲和性关系与涉及这些杂芳基哌嗪衍生物与5-HT(3)受体相互作用的关系的比较表明,选择性SERT / 5HT(3)受体的某些分子决定因素。

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