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The Predicted 3D Structure of Bitter Taste Receptors, TAS2R38 Based on a BiHelix and SuperBiHelix Methodologies

机译:基于Bihelix和Superbihelix方法的苦味受体的预测3D结构,TAS2R38

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TAS2R38 bitter taste receptors are seven-transmembrane (TM) domain G protein-coupled receptors (GPCRs) that can respond to bitter compounds such as Phenylthiocarbamide (PTC). We would like to understand the nature of the binding that is what aspect of the ligand interacting with the binding site leads to signal sent to the cortex. There are no direct determinations of the 3D structure of taste receptors; hence we use the new BiHelix and SuperBiHelix methods to predict the 3D structures of the TAS2R38 bitter taste receptors, which we chose because there is ample experimental data on how perception is related to the ligand and to mutations. These methods use a template to provide starting points for the structures and we tested four templates β1 Adrenergic Receptor (tβ1AR), β2 Adrenergic Receptor (hβ2AR), Bovine Rhodopsin and A2A Adenosine Receptor (hAA_(2A)R). We found the tβ1AR template is more appropriate for structural simulation of the bitter taste receptors. We predicted 3D structures of for four haplotypes PAV, AVI, AAI and PVV of the TAS2R38 bitter receptors. Our results illustrate that the residue 262 is involved in the interhelical hydrogen bond network stabilizing the structure in tasters (PAV, AAI and PVV) while it is not in non-tasters (AVI). Thus the hydrogen bond interaction between TM3 or TM5 and TM6 may play a role in activating this GPCR.
机译:Tas2R38苦味受体是七跨膜(TM)结构域G蛋白偶联受体(GPCR),其可以响应苦化合物,例如苯基硫代氨基甲酰胺(PTC)。我们想了解与结合位点相互作用的配体的哪个方面的性质导致发送到皮质的信号。味觉受体的3D结构没有直接确定;因此,我们使用新的Bihelix和Superbihelix方法来预测Tas2R38苦味受体的3D结构,我们选择了,因为有充分的实验数据是关于感知如何与配体相关和突变。这些方法使用模板提供结构的起点,并且我们测试了四个模板β1肾上腺素能受体(Tβ1AR),β2肾上腺素能受体(Hβ1AR),牛罗二糖蛋白酶和A2A腺苷受体(Haa_(2a)r)。我们发现Tβ1AR模板更适合于苦味受体的结构模拟。我们预测了TAS2R38苦受体的四个单倍型PAV,AVI,AAI和PVV的3D结构。我们的结果表明,残留物262涉及稳定味道(PAV,AAI和PVV)中结构的互臼氢键网络,同时不在非品尝者(AVI)中。因此,TM3或TM5和TM6之间的氢键相互作用可以发挥激活该GPCR的作用。

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