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人类嗅觉受体OR1A1和OR1A2对气味剂识别的结构决定因素。

Structural determinants of odorant recognition by the human olfactory receptors OR1A1 and OR1A2.

作者信息

Schmiedeberg Kristin, Shirokova Elena, Weber Hans-Peter, Schilling Boris, Meyerhof Wolfgang, Krautwurst Dietmar

机构信息

German Institute of Human Nutrition, Potsdam-Rehbruecke, Department of Molecular Genetics, Arthur-Scheunert-Allee 114-116, 14558 Nuthetal, Germany.

出版信息

J Struct Biol. 2007 Sep;159(3):400-12. doi: 10.1016/j.jsb.2007.04.013. Epub 2007 May 25.

Abstract

An interaction of odorants with olfactory receptors is thought to be the initial step in odorant detection. However, ligands have been reported for only 6 out of 380 human olfactory receptors, with their structural determinants of odorant recognition just beginning to emerge. Guided by the notion that amino acid positions that interact with specific odorants would be conserved in orthologs, but variable in paralogs, and based on the prediction of a set of 22 of such amino acid positions, we have combined site-directed mutagenesis, rhodopsin-based homology modelling, and functional expression in HeLa/Olf cells of receptors OR1A1 and OR1A2. We found that (i) their odorant profiles are centred around citronellic terpenoid structures, (ii) two evolutionary conserved amino acid residues in transmembrane domain 3 are necessary for the responsiveness of OR1A1 and the mouse ortholog Olfr43 to (S)-(-)-citronellol, (iii) changes at these two positions are sufficient to account for the differential (S)-(-)-citronellol responsiveness of the paralogs OR1A1 and OR1A2, and (iv) the interaction sites for (S)-(-)-citronellal and (S)-(-)-citronellol differ in both human receptors. Our results show that the orientation of odorants within a homology modelling-derived binding pocket of olfactory receptor orthologs is defined by evolutionary conserved amino acid positions.

摘要

气味分子与嗅觉受体的相互作用被认为是气味检测的第一步。然而,在380种人类嗅觉受体中,仅报道了6种的配体,其气味分子识别的结构决定因素才刚刚开始显现。基于与特定气味分子相互作用的氨基酸位置在直系同源物中保守但在旁系同源物中可变这一概念,并基于对一组22个此类氨基酸位置的预测,我们结合了定点诱变、基于视紫红质的同源建模以及受体OR1A1和OR1A2在HeLa/Olf细胞中的功能表达。我们发现:(i)它们的气味分子谱以香茅萜类结构为中心;(ii)跨膜结构域3中两个进化保守的氨基酸残基对于OR1A1和小鼠直系同源物Olfr43对(S)-(-)-香茅醇的反应性是必需的;(iii)这两个位置的变化足以解释旁系同源物OR1A1和OR1A2对(S)-(-)-香茅醇的不同反应性;(iv)在两种人类受体中,(S)-(-)-香茅醛和(S)-(-)-香茅醇的相互作用位点不同。我们的结果表明,嗅觉受体直系同源物的同源建模衍生结合口袋内气味分子的取向由进化保守的氨基酸位置定义。

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