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在V(H)3 Ig上绘制HIV-1 gp120的B细胞超抗原结合位点图谱。

Mapping the B cell superantigen binding site for HIV-1 gp120 on a V(H)3 Ig.

作者信息

Neshat M N, Goodglick L, Lim K, Braun J

机构信息

Department of Pathology and Laboratory Medicine, and The Molecular Biology Institute, University of California-Los Angeles, 10833 Le Conte Avenue, Los Angeles, CA 90095-1732, USA.

出版信息

Int Immunol. 2000 Mar;12(3):305-12. doi: 10.1093/intimm/12.3.305.

Abstract

The emerging class of B cell superantigens includes HIV-1 gp120, which binds to many members of the V(H)3 Ig gene family. The present study addresses the structural features of V(H)3 antibodies conferring gp120 binding activity using a panel of recombinant full-length and Fab Ig proteins. Binding activity was fully conferred by the Fab portion of the Ig molecule. The V(H) region was the major determinant of binding; diverse light chains were permissive for gp120 binding. A series of recombinant V(H)3-V(H)1 chimeric molecules was created to analyze the contribution of different subregions of V(H)3 to gp120 binding. Hypervariable loop 1 (H1) substitution alone caused a 10-fold reduction in binding activity. The framework subregions (FR1, FR2 and FR3) and H2 also influenced binding, since substitutions of various combinations of these subregions conferred 10- to 100-fold binding reductions. We conclude that gp120 binding occurs through a non-conventional interaction involving multiple discontinuously arrayed residues spanning the V(H), and including roles in gp120 contact and favorable conformation of the V(H).

摘要

新兴的B细胞超抗原类别包括HIV-1 gp120,它可与V(H)3 Ig基因家族的许多成员结合。本研究使用一组重组全长和Fab Ig蛋白,探讨了赋予gp120结合活性的V(H)3抗体的结构特征。结合活性完全由Ig分子的Fab部分赋予。V(H)区域是结合的主要决定因素;不同的轻链对gp120结合具有容许性。构建了一系列重组V(H)3-V(H)1嵌合分子,以分析V(H)3不同亚区域对gp120结合的贡献。仅高变环1(H1)替换就导致结合活性降低10倍。构架亚区域(FR1、FR2和FR3)以及H2也影响结合,因为这些亚区域各种组合的替换导致结合减少10至100倍。我们得出结论,gp120结合是通过一种非常规相互作用发生的,该相互作用涉及跨越V(H)的多个不连续排列的残基,并且包括在gp120接触和V(H)的有利构象中的作用。

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