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降钙素基因相关肽受体C端的功能与生物物理分析;B族G蛋白偶联受体

Functional and biophysical analysis of the C-terminus of the CGRP-receptor; a family B GPCR.

作者信息

Conner Matthew, Hicks Matthew R, Dafforn Tim, Knowles Timothy J, Ludwig Christian, Staddon Susan, Overduin Michael, Günther Ulrich L, Thome Johannes, Wheatley Mark, Poyner David R, Conner Alex C

机构信息

School of Biosciences, University of Birmingham, UK.

出版信息

Biochemistry. 2008 Aug 12;47(32):8434-44. doi: 10.1021/bi8004126. Epub 2008 Jul 18.

DOI:10.1021/bi8004126
PMID:18636754
Abstract

G-protein coupled receptors (GPCRs) typically have a functionally important C-terminus which, in the largest subfamily (family A), includes a membrane-parallel eighth helix. Mutations of this region are associated with several diseases. There are few C-terminal studies on the family B GPCRs and no data supporting the existence of a similar eighth helix in this second major subfamily, which has little or no sequence homology to family A GPCRs. Here we show that the C-terminus of a family B GPCR (CLR) has a disparate region from N400 to C436 required for CGRP-mediated internalization, and a proximal region of twelve residues (from G388 to W399), in a similar position to the family A eighth helix, required for receptor localization at the cell surface. A combination of circular and linear dichroism, fluorescence and modified waterLOGSY NMR spectroscopy (SALMON) demonstrated that a peptide mimetic of this domain readily forms a membrane-parallel helix anchored to the liposome by an interfacial tryptophan residue. The study reveals two key functions held within the C-terminus of a family B GPCR and presents support for an eighth helical region with striking topological similarity to the nonhomologous family A receptor. This helix structure appears to be found in most other family B GPCRs.

摘要

G蛋白偶联受体(GPCRs)通常具有功能上重要的C末端,在最大的亚家族(A家族)中,该末端包含一个与膜平行的第八螺旋。该区域的突变与多种疾病有关。关于B家族GPCRs的C末端研究较少,且没有数据支持在这个与A家族GPCRs几乎没有序列同源性的第二大亚家族中存在类似的第八螺旋。在这里,我们表明B家族GPCR(CLR)的C末端有一个从N400到C436的不同区域,这是降钙素基因相关肽(CGRP)介导内化所必需的,还有一个由十二个残基组成的近端区域(从G388到W399),其位置与A家族的第八螺旋相似,是受体定位在细胞表面所必需的。圆二色性和线性二色性、荧光以及改进的水LOGSY核磁共振光谱(SALMON)相结合表明,该结构域的肽模拟物很容易形成一个通过界面色氨酸残基锚定在脂质体上的与膜平行的螺旋。该研究揭示了B家族GPCR的C末端所具有的两个关键功能,并支持了一个与非同源A家族受体具有显著拓扑相似性的第八螺旋区域。这种螺旋结构似乎在大多数其他B家族GPCR中都存在。

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