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B淋巴细胞、固有免疫与自身免疫

B-lymphocytes, innate immunity, and autoimmunity.

作者信息

Viau Muriel, Zouali Moncef

机构信息

Institut National de Santé et de Recherche Médicale (INSERM U 430), Immunopathologie Humaine, 75006 Paris, France.

出版信息

Clin Immunol. 2005 Jan;114(1):17-26. doi: 10.1016/j.clim.2004.08.019.

DOI:10.1016/j.clim.2004.08.019
PMID:15596405
Abstract

Having evolved to generate a huge Ag-specific repertoire and to mount T cell-dependent responses and long-term memory, the B lymphocyte is a central player in the adaptive branch of immune defense. However, accumulating evidence indicates that B-1 cells of the peritoneal cavity and marginal zone (MZ) B cells of the spleen also can play innate-like immune functions. Their anatomical locations allow frequent Ag encounter. Secreting essentially germline-encoded, polyreactive Abs, and responding rapidly and vigorously to stimulation, these two B cell subsets have evolved to impart potentially protective responses. With their additional capacities to secrete factors that can directly mediate microbial destruction and to express Toll-like receptors (TLR), B cells provide an important link between the innate and adaptive branches of the immune system. Currently, the relevance of these innate-like B cells to the pathogenesis of autoimmune disease is the focus of investigation. In experimental models of autoimmunity, the sequestration of autoreactive B cells in the MZ has been proposed to be essential for the maintenance of self-tolerance. The low activation threshold of MZ B cells makes them particularly reactive to high loads and/or altered self-Ags, potentially exacerbating autoimmune disease. Their expansion in autoimmune models and their association with autoantibody secretion indicate that they may participate in tissue damage. The demonstration that B cell depletion therapies may represent a highly beneficial therapeutic goal in autoimmune disorders suggests that specific elimination of B-1 and MZ B cells may represent a more efficient immunointervention strategy in systemic autoimmunity.

摘要

B淋巴细胞经过进化,能够产生庞大的抗原特异性库,引发T细胞依赖性反应并形成长期记忆,是免疫防御适应性分支中的核心角色。然而,越来越多的证据表明,腹腔中的B-1细胞和脾脏边缘区(MZ)B细胞也能发挥类先天性免疫功能。它们的解剖位置使其频繁接触抗原。这两个B细胞亚群分泌基本由种系编码的多反应性抗体,并对刺激迅速而强烈地做出反应,进化出了可能具有保护作用的反应。B细胞还具有分泌可直接介导微生物破坏的因子以及表达Toll样受体(TLR)的额外能力,在免疫系统的先天性和适应性分支之间提供了重要联系。目前,这些类先天性B细胞与自身免疫性疾病发病机制的相关性是研究的重点。在自身免疫性疾病的实验模型中,有人提出将自身反应性B细胞隔离在边缘区对于维持自身耐受性至关重要。边缘区B细胞的低激活阈值使其对高负荷和/或改变的自身抗原特别敏感,可能会加剧自身免疫性疾病。它们在自身免疫模型中的扩增以及与自身抗体分泌的关联表明它们可能参与组织损伤。B细胞清除疗法可能是自身免疫性疾病中一个非常有益的治疗目标,这一证明表明,特异性清除B-1细胞和边缘区B细胞可能是全身性自身免疫中一种更有效的免疫干预策略。

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