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人类神经肽 S 受体及其拮抗剂的分子建模研究。

Molecular modeling studies on the human neuropeptide S receptor and its antagonists.

机构信息

Dipartimento di Scienze Chimiche, Università di Camerino, Via S. Agostino 1, 62032 Camerino, MC, Italy.

出版信息

ChemMedChem. 2010 Mar 1;5(3):371-83. doi: 10.1002/cmdc.200900467.

Abstract

Neuropeptide S (NPS) is a 20-residue peptide of great interest due to its potential involvement in several biological processes such as arousal, anxiety, and food intake. The NPS receptor belongs to the rhodopsin-like G-protein-coupled receptor superfamily, and several polymorphisms and isoforms of this receptor are associated with asthma, allergies, and bronchial hyper-responsiveness, in particular the Asn 107 Ile mutation. Limited structural information is available for this peptide-receptor system, particularly regarding the NPS receptor structure, its nonpeptide ligands, and the molecular aspects of agonist and antagonist binding processes. In this work, rhodopsin-based homology models of the NPS receptor and its Asn 107 Ile variant were built and refined in a membrane bilayer model, and binding modes for nonpeptide antagonists were simulated. This study provides the first structural study of the human NPS receptor, and the results provide a starting point for further characterization of the binding modes of its antagonists, and for the rational design of new NPS receptor ligands.

摘要

神经肽 S(NPS)是一种 20 个氨基酸的肽,由于其可能参与多种生物学过程,如觉醒、焦虑和食物摄入,因此备受关注。NPS 受体属于视紫红质样 G 蛋白偶联受体超家族,该受体的几种多态性和同工型与哮喘、过敏和支气管高反应性有关,特别是 Asn107Ile 突变。关于该肽 - 受体系统,特别是 NPS 受体结构、其非肽配体以及激动剂和拮抗剂结合过程的分子方面,目前仅有有限的结构信息。在这项工作中,构建并在双层膜模型中优化了 NPS 受体及其 Asn107Ile 变体的基于视紫红质的同源模型,并模拟了非肽拮抗剂的结合模式。该研究首次对人 NPS 受体进行了结构研究,研究结果为进一步研究其拮抗剂的结合模式以及合理设计新型 NPS 受体配体提供了起点。

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