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神经递质转运体的三维模型及其与可卡因和S-西酞普兰的相互作用。

Three-dimensional models of neurotransmitter transporters and their interactions with cocaine and S-citalopram.

作者信息

Ravna Aina Westrheim

机构信息

Department of Pharmacology, Institute of Medical Biology, University of Tromsø, Tromsø, Norway.

出版信息

World J Biol Psychiatry. 2006;7(2):99-109. doi: 10.1080/15622970500402144.

Abstract

Drugs that act on the human serotonin transporter (hSERT), human dopamine transporter (hDAT) and human noradrenaline transporter (hNET) are important in antidepressant treatment and well known in drug abuse. The investigation of their molecular mechanisms of action is very useful for designing new ligands with a therapeutic potential. The detailed three-dimensional molecular structure of any monoamine transporter is not known, but the three-dimensional electron density projection map of Escherichia coli Na+/H+ antiporter (NhaA) has provided structural basis for constructing models of such transporters using molecular modelling techniques. Three-dimensional models of these drug targets give insight into their structure, mechanisms and drug interactions. In these molecular modelling studies, an Escherichia coli NhaA model was first constructed based on its three-dimensional electron density projection map and experimental studies on NhaA and the Escherichia coli lactose permease symporter (Lac permease). Then three-dimensional models of the neurotransmitter transporters hDAT, hSERT and hNET were constructed based on the NhaA model and studies of ligand binding to mutated dopamine transporter (DAT) and serotonin transporter (SERT). The structural properties of these neurotransmitter transporter models have been examined, and their interactions with cocaine and S-citalopram have been investigated.

摘要

作用于人类5-羟色胺转运体(hSERT)、人类多巴胺转运体(hDAT)和人类去甲肾上腺素转运体(hNET)的药物在抗抑郁治疗中很重要,且在药物滥用方面广为人知。对其作用分子机制的研究对于设计具有治疗潜力的新配体非常有用。尚不清楚任何单胺转运体的详细三维分子结构,但大肠杆菌Na+/H+反向转运蛋白(NhaA)的三维电子密度投影图为使用分子建模技术构建此类转运体模型提供了结构基础。这些药物靶点的三维模型有助于深入了解其结构、机制和药物相互作用。在这些分子建模研究中,首先基于大肠杆菌NhaA的三维电子密度投影图以及对NhaA和大肠杆菌乳糖通透酶同向转运体(乳糖通透酶)的实验研究构建了大肠杆菌NhaA模型。然后基于NhaA模型以及配体与突变多巴胺转运体(DAT)和5-羟色胺转运体(SERT)结合的研究构建了神经递质转运体hDAT、hSERT和hNET的三维模型。已对这些神经递质转运体模型的结构特性进行了研究,并研究了它们与可卡因和S-西酞普兰的相互作用。

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