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葡萄球菌肠毒素A通过与VH区低亲和力结合诱导表达VH3的人B细胞存活。

Staphylococcal enterotoxin A induces survival of VH3-expressing human B cells by binding to the VH region with low affinity.

作者信息

Domiati-Saad R, Lipsky P E

机构信息

Department of Internal Medicine, Harold C. Simmons Arthritis Research Center, University of Texas Southwestern Medical Center, Dallas 75235-8884, USA.

出版信息

J Immunol. 1998 Aug 1;161(3):1257-66.

PMID:9686586
Abstract

Staphylococcal enterotoxins (SE) are bacterial superantigens that bind to MHC class II molecules and to the V beta-chain of the TCR, and subsequently activate T cells expressing specific V beta regions. In this study, we have studied the effects of SEA on human B cell activation, and specifically the capacity of SEA to function as a B cell superantigen in vitro. We show herein that SEA failed to induce B cell proliferation and differentiation in the absence of T cells. However, SEA induced survival of B cells uniquely expressing VH3-containing IgM, independently of light chain utilization. The sequences of VH3 IgM gene products were determined and found to include a number of members of the VH3 family with a variety of different D and JH gene segments. Analysis of the sequences of VH3 gene products revealed possible sites in framework region 1 and/or framework region 3 that could be involved in SEA-mediated activation of VH3-expressing B cells. Binding studies showed that SEA interacts with the VH3 domain of Ig with low, but detectable affinity. These results indicate that SEA functions as a B cell superantigen by interacting with VH3 gene segments of Ig.

摘要

葡萄球菌肠毒素(SE)是一类细菌超抗原,可与MHC II类分子及T细胞受体的Vβ链结合,随后激活表达特定Vβ区域的T细胞。在本研究中,我们研究了SEA对人B细胞活化的影响,特别是SEA在体外作为B细胞超抗原发挥作用的能力。我们在此表明,在没有T细胞的情况下,SEA无法诱导B细胞增殖和分化。然而,SEA可诱导独特表达含VH3的IgM的B细胞存活,而与轻链的利用无关。测定了VH3 IgM基因产物的序列,发现其中包括VH3家族的多个成员,带有多种不同的D和JH基因片段。对VH3基因产物序列的分析揭示了框架区1和/或框架区3中可能参与SEA介导的表达VH3的B细胞活化的位点。结合研究表明,SEA与Ig的VH3结构域以低但可检测到的亲和力相互作用。这些结果表明,SEA通过与Ig的VH3基因片段相互作用而作为B细胞超抗原发挥作用。

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