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B细胞超抗原:定义及其对免疫反应的潜在影响。

B-cell superantigens: definition and potential impact on the immune response.

作者信息

Levinson A I, Kozlowski L, Zheng Y, Wheatley L

机构信息

Division of Allergy and Immunology, University of Pennsylvania School of Medicine, Philadelphia 19104, USA.

出版信息

J Clin Immunol. 1995 Nov;15(6 Suppl):26S-36S. doi: 10.1007/BF01540891.

Abstract

Superantigens have been extremely helpful tools in exploring fundamental questions in immunobiology including mechanisms of cell activation, tolerance, and autoimmunity. Until recently, attention has been focused exclusive on T-cell superantigens. However, new data suggest that there are superantigens that directly activate B cells. By definition, these agents (1) stimulate a high frequency of B cells, (2) target B cells that have restricted usage of VH or VL family genes, and (3) bind to immunoglobulins outside the sites that bind conventional antigens. A candidate B-cell superantigen that has received considerable attention in this laboratory is staphylococcal protein A. This agent is best known to the immunologist because of its ability to bind to the Fc fragment of IgG. This binding has been localized to two alpha-helical structures on each of four or five homologous regions that comprise the extracellular domain of protein A. However, it is now clear that protein A contains a second site that binds to determinants on the Fab regions of certain immunoglobulins independently of their heavy-chain isotype. In man this so-called alternative site appears to bind only to immunoglobulins that utilize heavy-chain genes of the VH3 subfamily. In the mouse this type of binding is restricted to immunoglobulins using heavy chains belonging to the S107 and J606 VH families. In this review, we examine the growing list of microbial products that dominate B-cell superantigenic properties. Using staphylococcal protein A as a model for a B-cell superantigen, we consider the potential impact of this novel class of antigens on the immune response. We focus on the ability of B-cell superantigens to influence the expression of the B-cell repertoire. In addition, we consider the hypothesis that the interaction of a B-cell superantigen with its reactive serum immunoglobulins activates the classical complement cascade and thus represents a powerful stimulant of tissue inflammation.

摘要

超抗原在探索免疫生物学的基本问题(包括细胞活化、耐受和自身免疫机制)方面一直是极为有用的工具。直到最近,人们的注意力一直完全集中在T细胞超抗原上。然而,新数据表明存在直接激活B细胞的超抗原。根据定义,这些因子(1)刺激高频率的B细胞,(2)靶向VH或VL家族基因使用受限的B细胞,并且(3)结合在结合常规抗原的位点之外的免疫球蛋白。在本实验室中受到相当多关注的一种候选B细胞超抗原是葡萄球菌蛋白A。免疫学家对这种因子最为了解,因为它能够结合IgG的Fc片段。这种结合已定位到构成蛋白A细胞外结构域的四或五个同源区域中每个区域的两个α螺旋结构上。然而,现在清楚的是,蛋白A含有第二个位点,该位点独立于其重链同种型与某些免疫球蛋白的Fab区域上的决定簇结合。在人类中,这个所谓的替代位点似乎仅结合利用VH3亚家族重链基因的免疫球蛋白。在小鼠中,这种结合类型仅限于使用属于S107和J606 VH家族重链的免疫球蛋白。在这篇综述中,我们研究了越来越多具有B细胞超抗原特性的微生物产物。以葡萄球菌蛋白A作为B细胞超抗原的模型,我们考虑这类新型抗原对免疫反应的潜在影响。我们关注B细胞超抗原影响B细胞库表达的能力。此外,我们考虑这样一种假说,即B细胞超抗原与其反应性血清免疫球蛋白的相互作用激活经典补体级联反应,因此代表了组织炎症的强大刺激物。

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