B cell superantigens: a microbe's answer to innate-like B cells and natural antibodies.

Carl S Goodyear, Gregg J Silverman
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引用次数: 49

Abstract

Marginal zone B cells and B-1 cells have been termed innate-like B cells as they express limited repertoires that play special roles in immune defenses against common infections. These B cells are the sources of natural antibodies and are capable of highly accelerated clonal responses that help counter blood-borne infections. We have characterized a class of microbial product with highly adapted binding interactions with host immunoglobulins/B cell receptors (BCRs), which enable the targeting of large supra-clonal sets of B cells for activation-associated apoptotic death. In recent studies, we have shown that all B cells with V region-targeted BCRs are susceptible. However, compared to follicular B cells, in vivo exposure preferentially causes innate-like B cells to undergo induced death with subsequent long-lasting supra-clonal depletion and immune tolerance. Based on these properties, it is likely that B cell superantigens influence the pathogenesis of some common infections, but also may provide novel therapeutic opportunities to treat B cell neoplastic and autoimmune diseases.

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B细胞超级抗原:一种微生物对先天B细胞和天然抗体的应答。
边缘区B细胞和B-1细胞被称为先天样B细胞,因为它们表达有限的基因库,在对抗常见感染的免疫防御中发挥特殊作用。这些B细胞是天然抗体的来源,能够高度加速克隆反应,帮助对抗血源性感染。我们已经鉴定了一类微生物产物,它们与宿主免疫球蛋白/B细胞受体(bcr)具有高度适应性的结合相互作用,能够靶向大量超克隆B细胞,以实现激活相关的凋亡死亡。在最近的研究中,我们发现所有具有V区靶向bcr的B细胞都是易感的。然而,与滤泡B细胞相比,体内暴露优先导致先天样B细胞诱导死亡,随后出现长期的超克隆耗竭和免疫耐受。基于这些特性,B细胞超抗原可能影响一些常见感染的发病机制,但也可能为治疗B细胞肿瘤和自身免疫性疾病提供新的治疗机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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