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猴免疫缺陷病毒糖蛋白41(SIV gp41)44 kDa胞外域的三维溶液结构

Three-dimensional solution structure of the 44 kDa ectodomain of SIV gp41.

作者信息

Caffrey M, Cai M, Kaufman J, Stahl S J, Wingfield P T, Covell D G, Gronenborn A M, Clore G M

机构信息

Laboratory of Chemical Physics, Building 5, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892-0520, USA.

出版信息

EMBO J. 1998 Aug 17;17(16):4572-84. doi: 10.1093/emboj/17.16.4572.

Abstract

The solution structure of the ectodomain of simian immunodeficiency virus (SIV) gp41 (e-gp41), consisting of residues 27-149, has been determined by multidimensional heteronuclear NMR spectroscopy. SIV e-gp41 is a symmetric 44 kDa trimer with each subunit consisting of antiparallel N-terminal (residues 30-80) and C-terminal (residues 107-147) helices connected by a 26 residue loop (residues 81-106). The N-terminal helices of each subunit form a parallel coiled-coil structure in the interior of the complex which is surrounded by the C-terminal helices located on the exterior of the complex. The loop region is ordered and displays numerous intermolecular and non-sequential intramolecular contacts. The helical core of SIV e-gp41 is similar to recent X-ray structures of truncated constructs of the helical core of HIV-1 e-gp41. The present structure establishes unambiguously the connectivity of the N- and C-terminal helices in the trimer, and characterizes the conformation of the intervening loop, which has been implicated by mutagenesis and antibody epitope mapping to play a key role in gp120 association. In conjunction with previous studies, the solution structure of the SIV e-gp41 ectodomain provides insight into the binding site of gp120 and the mechanism of cell fusion. The present structure of SIV e-gp41 represents one of the largest protein structures determined by NMR to date.

摘要

通过多维异核核磁共振光谱法,已确定了猿猴免疫缺陷病毒(SIV)gp41胞外域(e-gp41,由27至149位氨基酸残基组成)的溶液结构。SIV e-gp41是一个对称的44 kDa三聚体,每个亚基由反平行的N端螺旋(30至80位氨基酸残基)和C端螺旋(107至147位氨基酸残基)组成,二者由一个26个氨基酸残基的环(81至106位氨基酸残基)相连。每个亚基的N端螺旋在复合物内部形成一个平行卷曲螺旋结构,该结构被位于复合物外部的C端螺旋包围。环区域有序排列,并显示出大量分子间和非连续分子内接触。SIV e-gp41的螺旋核心与HIV-1 e-gp41螺旋核心的截短构建体的近期X射线结构相似。目前的结构明确地确定了三聚体中N端和C端螺旋的连接性,并表征了中间环的构象,该环通过诱变和抗体表位作图被认为在gp120结合中起关键作用。结合先前的研究,SIV e-gp41胞外域的溶液结构为深入了解gp120的结合位点和细胞融合机制提供了线索。目前SIV e-gp41的结构代表了迄今为止通过核磁共振确定的最大蛋白质结构之一。

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