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鉴定对中毒性休克综合征毒素超抗原结合至关重要的HLA - DRα链残基。

Identification of HLA-DR alpha chain residues critical for binding of the toxic shock syndrome toxin superantigen.

作者信息

Panina-Bordignon P, Fu X T, Lanzavecchia A, Karr R W

机构信息

Basel Institute for Immunology, Switzerland.

出版信息

J Exp Med. 1992 Dec 1;176(6):1779-84. doi: 10.1084/jem.176.6.1779.

Abstract

Staphylococcal toxic shock syndrome toxin 1 (TSST-1) binds to major histocompatibility complex class II molecules, and the toxin-class II complexes induce proliferation of T cells expressing V beta 2 sequences. To define the residues involved in TSST-1 binding, a set of transfectants expressing 21 HLA-DR alpha chain mutants were analyzed for their abilities to bind and present TSST-1 and to present an antigenic peptide. Mutations at DR alpha positions 36 and 39 markedly decreased the ability of the DR7 molecule to bind and present TSST-1 but did not affect the ability to present an antigenic peptide. These data indicate that DR alpha residues 36 and 39, predicted to be located on an outer loop, are important in the formation of the TSST-1 binding site on DR molecules.

摘要

葡萄球菌中毒性休克综合征毒素1(TSST-1)与主要组织相容性复合体II类分子结合,毒素 - II类复合物诱导表达Vβ2序列的T细胞增殖。为了确定参与TSST-1结合的残基,分析了一组表达21种HLA-DRα链突变体的转染子结合和呈递TSST-1以及呈递抗原肽的能力。DRα位置36和39处的突变显著降低了DR7分子结合和呈递TSST-1的能力,但不影响呈递抗原肽的能力。这些数据表明,预测位于外环上的DRα残基36和39在DR分子上TSST-1结合位点的形成中很重要。

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