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哺乳动物嗅觉受体建模与气味剂对接

Modeling of mammalian olfactory receptors and docking of odorants.

作者信息

Launay Guillaume, Sanz Guenhaël, Pajot-Augy Edith, Gibrat Jean-François

机构信息

Equipe interactions hôte-pathogène, Bases Moléculaires et Structurales des Systèmes Infectieux, UMR5086 CNRS/Université de Lyon1, 7 Passage du Vercors, Lyon cedex 07, France.

Neurobiologie de l'Olfaction et Modélisation en Imagerie UR1197, INRA, 78350, Jouy-en-Josas, France.

出版信息

Biophys Rev. 2012 Sep;4(3):255-269. doi: 10.1007/s12551-012-0080-0. Epub 2012 Sep 1.

Abstract

Olfactory receptors (ORs) belong to the superfamily of G protein-coupled receptors (GPCRs), the second largest class of genes after those related to immunity, and account for about 3 % of mammalian genomes. ORs are present in all multicellular organisms and represent more than half the GPCRs in mammalian species (e.g., the mouse OR repertoire contains >1,000 functional genes). ORs are mainly expressed in the olfactory epithelium where they detect odorant molecules, but they are also expressed in a number of other cells, such as sperm cells, although their functions in these cells remain mostly unknown. It has recently been reported that ORs are present in tumoral tissues where they are expressed at different levels than in healthy tissues. A specific OR is over-expressed in prostate cancer cells, and activation of this OR has been shown to inhibit the proliferation of these cells. Odorant stimulation of some of these receptors results in inhibition of cell proliferation. Even though their biological role has not yet been elucidated, these receptors might constitute new targets for diagnosis and therapeutics. It is important to understand the activation mechanism of these receptors at the molecular level, in particular to be able to predict which ligands are likely to activate a particular receptor ('deorphanization') or to design antagonists for a given receptor. In this review, we describe the in silico methodologies used to model the three-dimensional (3D) structure of ORs (in the more general framework of GPCR modeling) and to dock ligands into these 3D structures.

摘要

嗅觉受体(ORs)属于G蛋白偶联受体(GPCRs)超家族,是仅次于免疫相关基因的第二大基因类别,约占哺乳动物基因组的3%。ORs存在于所有多细胞生物中,在哺乳动物物种中占GPCRs的一半以上(例如,小鼠的OR库包含超过1000个功能基因)。ORs主要表达于嗅觉上皮,在那里它们检测气味分子,但也在许多其他细胞中表达,如精子细胞,尽管它们在这些细胞中的功能大多仍不清楚。最近有报道称,ORs存在于肿瘤组织中,其表达水平与健康组织不同。一种特定的OR在前列腺癌细胞中过度表达,并且已证明激活该OR可抑制这些细胞的增殖。对其中一些受体的气味刺激会导致细胞增殖受到抑制。尽管它们的生物学作用尚未阐明,但这些受体可能构成诊断和治疗的新靶点。重要的是要在分子水平上了解这些受体的激活机制,特别是能够预测哪些配体可能激活特定受体(“去孤儿化”)或为给定受体设计拮抗剂。在这篇综述中,我们描述了用于模拟ORs三维(3D)结构(在GPCR建模的更一般框架内)以及将配体对接至这些3D结构的计算机模拟方法。

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