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苦味受体 TAS2R16 通过使用双面结合口袋实现高特异性和容纳多种糖苷配体。

The Bitter Taste Receptor TAS2R16 Achieves High Specificity and Accommodates Diverse Glycoside Ligands by using a Two-faced Binding Pocket.

机构信息

Integral Molecular, Inc., 3711 Market St, Suite 900, Philadelphia, PA, 19104, USA.

出版信息

Sci Rep. 2017 Aug 10;7(1):7753. doi: 10.1038/s41598-017-07256-y.

Abstract

Although bitter taste receptors (TAS2Rs) are important for human health, little is known of the determinants of ligand specificity. TAS2Rs such as TAS2R16 help define gustatory perception and dietary preferences that ultimately influence human health and disease. Each TAS2R must accommodate a broad diversity of chemical structures while simultaneously achieving high specificity so that diverse bitter toxins can be detected without all foods tasting bitter. However, how these G protein-coupled receptors achieve this balance is poorly understood. Here we used a comprehensive mutation library of human TAS2R16 to map its interactions with existing and novel agonists. We identified 13 TAS2R16 residues that contribute to ligand specificity and 38 residues whose mutation eliminated signal transduction by all ligands, providing a comprehensive assessment of how this GPCR binds and signals. Our data suggest a model in which hydrophobic residues on TM3 and TM7 form a broad ligand-binding pocket that can accommodate the diverse structural features of β-glycoside ligands while still achieving high specificity.

摘要

尽管苦味受体(TAS2R)对人类健康很重要,但对于配体特异性的决定因素知之甚少。TAS2R16 等 TAS2R 有助于定义味觉感知和饮食偏好,最终影响人类健康和疾病。每个 TAS2R 都必须适应广泛的化学结构多样性,同时实现高度特异性,以便在不使所有食物都具有苦味的情况下检测到不同的苦味毒素。然而,这些 G 蛋白偶联受体如何实现这种平衡还知之甚少。在这里,我们使用了人类 TAS2R16 的综合突变文库来绘制其与现有和新型激动剂的相互作用。我们确定了 13 个 TAS2R16 残基有助于配体特异性,还有 38 个残基的突变消除了所有配体的信号转导,从而全面评估了这种 GPCR 如何结合和发出信号。我们的数据表明,TM3 和 TM7 上的疏水性残基形成了一个广泛的配体结合口袋,可以容纳β-糖苷配体的各种结构特征,同时仍然实现高度特异性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8eff/5552880/c9a92c9c9fdb/41598_2017_7256_Fig1_HTML.jpg

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