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苯基硫脲和丙基硫氧嘧啶苦味感知个体差异的分子基础。

The molecular basis of individual differences in phenylthiocarbamide and propylthiouracil bitterness perception.

作者信息

Bufe Bernd, Breslin Paul A S, Kuhn Christina, Reed Danielle R, Tharp Christopher D, Slack Jay P, Kim Un-Kyung, Drayna Dennis, Meyerhof Wolfgang

机构信息

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

出版信息

Curr Biol. 2005 Feb 22;15(4):322-7. doi: 10.1016/j.cub.2005.01.047.

Abstract

Individual differences in perception are ubiquitous within the chemical senses: taste, smell, and chemical somesthesis . A hypothesis of this fact states that polymorphisms in human sensory receptor genes could alter perception by coding for functionally distinct receptor types . We have previously reported evidence that sequence variants in a presumptive bitter receptor gene (hTAS2R38) correlate with differences in bitterness recognition of phenylthiocarbamide (PTC) . Here, we map individual psychogenomic pathways for bitter taste by testing people with a variety of psychophysical tasks and linking their individual perceptions of the compounds PTC and propylthiouracil (PROP) to the in vitro responses of their TAS2R38 receptor variants. Functional expression studies demonstrate that five different haplotypes from the hTAS2R38 gene code for operatively distinct receptors. The responses of the three haplotypes we also tested in vivo correlate strongly with individuals' psychophysical bitter sensitivities to a family of compounds. These data provide a direct molecular link between heritable variability in bitter taste perception to functional variations of a single G protein coupled receptor that responds to compounds such as PTC and PROP that contain the N-C=S moiety. The molecular mechanisms of perceived bitterness variability have therapeutic implications, such as helping patients to consume beneficial bitter-tasting compounds-for example, pharmaceuticals and selected phytochemicals.

摘要

在化学感官(味觉、嗅觉和化学本体感觉)中,个体在感知方面的差异普遍存在。关于这一事实的一种假说认为,人类感官受体基因的多态性可能通过编码功能不同的受体类型来改变感知。我们之前曾报道过证据,表明一种推测的苦味受体基因(hTAS2R38)中的序列变异与苯硫脲(PTC)苦味识别的差异相关。在这里,我们通过用各种心理物理学任务测试人们,并将他们对化合物PTC和丙基硫氧嘧啶(PROP)的个体感知与他们TAS2R38受体变体的体外反应联系起来,绘制出苦味的个体心理基因组途径。功能表达研究表明,hTAS2R38基因的五种不同单倍型编码功能不同的受体。我们在体内也测试的三种单倍型的反应与个体对一类化合物的心理物理苦味敏感性密切相关。这些数据提供了苦味感知的遗传变异性与单个G蛋白偶联受体的功能变异之间的直接分子联系,该受体对含有N-C=S部分的化合物(如PTC和PROP)有反应。感知苦味变异性的分子机制具有治疗意义,例如帮助患者食用有益的苦味化合物,如药物和某些植物化学物质。

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