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关键氨基酸改变了一个高度保守的嗅觉受体的活性和运输。

Key amino acids alter activity and trafficking of a well-conserved olfactory receptor.

机构信息

Department of Physiology, Johns Hopkins University School of Medicine, Baltimore, Maryland.

出版信息

Am J Physiol Cell Physiol. 2022 Jun 1;322(6):C1279-C1288. doi: 10.1152/ajpcell.00440.2021. Epub 2022 May 11.

Abstract

In this study, we elucidate factors that regulate the trafficking and activity of a well-conserved olfactory receptor (OR), olfactory receptor 558 (Olfr558), and its human ortholog olfactory receptor 51E1 (OR51E1). Results indicate that butyrate activates Olfr558/OR51E1 leading to the production of cAMP, and evokes Ca influx. We also find olfactory G protein (Golf) increases cAMP production induced by Olfr558/OR51E1 activation but does not affect trafficking. Given the 93% sequence identity between OR51E1 and Olfr558, it is surprising to note that OR51E1 has significantly more surface expression yet similar total protein expression. We find that replacing the Olfr558 N-terminus with that of OR51E1 significantly increases trafficking; in contrast, there is no change in surface expression conferred by the OR51E1 TM2, TM3, or TM4 domains. A previous analysis of human OR51E1 single nucleotide polymorphisms (SNPs) identified an A156T mutant primarily found in South Asia as the most abundant (albeit still rare). We find that the OR51E1 A156T mutant has reduced surface expression and cAMP production without a change in total protein expression. In sum, this study of a well-conserved olfactory receptor identifies both protein regions and specific amino acid residues that play key roles in protein trafficking and also elucidates common effects of Golf on the regulation of both the human and murine OR.

摘要

在这项研究中,我们阐明了调节嗅觉受体(OR)558(Olfr558)及其人类同源物 OR51E1(OR51E1)的运输和活性的因素。结果表明,丁酸激活 Olfr558/OR51E1 导致 cAMP 的产生,并引发 Ca2+内流。我们还发现嗅觉 G 蛋白(Golf)增加 Olfr558/OR51E1 激活引起的 cAMP 产生,但不影响运输。鉴于 OR51E1 和 Olfr558 之间 93%的序列同一性,令人惊讶的是,OR51E1 具有明显更高的表面表达,但总蛋白表达相似。我们发现用 OR51E1 的 N 端替换 Olfr558 的 N 端可显著增加运输;相比之下,OR51E1 的 TM2、TM3 或 TM4 结构域并没有赋予表面表达的变化。对人类 OR51E1 单核苷酸多态性(SNP)的先前分析确定了一个主要在南亚发现的 A156T 突变体,是最丰富的(尽管仍然很少)。我们发现 OR51E1 A156T 突变体的表面表达和 cAMP 产生减少,而总蛋白表达没有变化。总之,这项对保守嗅觉受体的研究确定了在蛋白质运输中起关键作用的蛋白质区域和特定氨基酸残基,并阐明了 Golf 对人类和鼠类 OR 调节的共同影响。

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