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通过人鼠比较预测嗅觉受体蛋白的气味结合位点

Prediction of the odorant binding site of olfactory receptor proteins by human-mouse comparisons.

作者信息

Man Orna, Gilad Yoav, Lancet Doron

机构信息

Department of Molecular Genetics and the Crown Human Genome Center, The Weizmann Institute of Science, Rehovot 76100, Israel.

出版信息

Protein Sci. 2004 Jan;13(1):240-54. doi: 10.1110/ps.03296404.

Abstract

Olfactory receptors (ORs) are a large family of proteins involved in the recognition and discrimination of numerous odorants. These receptors belong to the G-protein coupled receptor (GPCR) hyperfamily, for which little structural data are available. In this study we predict the binding site residues of OR proteins by analyzing a set of 1441 OR protein sequences from mouse and human. The central insight utilized is that functional contact residues would be conserved among pairs of orthologous receptors, but considerably less conserved among paralogous pairs. Using judiciously selected subsets of 218 ortholog pairs and 518 paralog pairs, we have identified 22 sequence positions that are both highly conserved among the putative orthologs and variable among paralogs. These residues are disposed on transmembrane helices 2 to 7, and on the second extracellular loop of the receptor. Strikingly, although the prediction makes no assumption about the location of the binding site, these amino acid positions are clustered around a pocket in a structural homology model of ORs, mostly facing the inner lumen. We propose that the identified positions constitute the odorant binding site. This conclusion is supported by the observation that all but one of the predicted binding site residues correspond to ligand-contact positions in other rhodopsin-like GPCRs.

摘要

嗅觉受体(ORs)是一个大家族的蛋白质,参与众多气味剂的识别和区分。这些受体属于G蛋白偶联受体(GPCR)超家族,目前关于其结构的数据很少。在本研究中,我们通过分析一组来自小鼠和人类的1441个OR蛋白序列,预测了OR蛋白的结合位点残基。所利用的核心观点是,功能接触残基在直系同源受体对之间是保守的,但在旁系同源对之间的保守性要低得多。通过明智地选择218对直系同源对和518对旁系同源对的子集,我们确定了22个序列位置,这些位置在假定的直系同源物中高度保守,而在旁系同源物中则可变。这些残基分布在跨膜螺旋2至7以及受体的第二个细胞外环上。引人注目的是,尽管预测并未对结合位点的位置做出假设,但这些氨基酸位置在ORs的结构同源模型中围绕一个口袋聚集,大多面向内腔。我们提出,所确定的位置构成了气味剂结合位点。这一结论得到了以下观察结果的支持:除一个预测的结合位点残基外,所有其他残基都对应于其他视紫红质样GPCR中的配体接触位置。

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