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针对凋亡细胞的保护性天然自身抗体:反复出现的固有样克隆趋同选择的证据。

Protective natural autoantibodies to apoptotic cells: evidence of convergent selection of recurrent innate-like clones.

作者信息

Silverman Gregg J

机构信息

Departments of Medicine and Pathology, NYU School of Medicine, Alexandria Center for Life Science, New York, New York.

出版信息

Ann N Y Acad Sci. 2015 Dec;1362(1):164-75. doi: 10.1111/nyas.12788. Epub 2015 May 18.

Abstract

During murine immune development, recurrent B cell clones arise in a predictable fashion. Among these B cells, an archetypical clonotypic set that recognizes phosphorylcholine (PC) antigens and produces anti-PC IgM, first implicated for roles in microbial protection, was later found to become expanded in hyperlipidemic mice and in response to an increased in vivo burden of apoptotic cells. These IgM natural antibodies can enhance clearance of damaged cells and induce intracellular blockade of inflammatory signaling cascades. In clinical populations, raised levels of anti-PC IgM correlate with protection from atherosclerosis and may also downmodulate the severity of autoimmune disease. Human anti-PC-producing clones without hypermutation have been isolated that can similarly discriminate apoptotic from healthy cells. An independent report on unrelated adults has described anti-PC-producing B cells with IgM genes that have conserved CDR3 motifs, similar to stereotypic clonal sets of B cell chronic lymphocytic leukemia. Taken together, emerging evidence suggests that, despite the capacity to form an effectively limitless range of Ig receptors, the human immune system may often recurrently generate lymphocytes expressing structurally convergent B cell receptors with protective and homeostatic roles.

摘要

在小鼠免疫发育过程中,反复出现的B细胞克隆以可预测的方式产生。在这些B细胞中,一组典型的克隆型细胞能够识别磷酸胆碱(PC)抗原并产生抗PC IgM,最初认为其在微生物保护中发挥作用,后来发现其在高脂血症小鼠中以及对体内凋亡细胞负担增加的反应中会扩增。这些IgM天然抗体可增强受损细胞的清除,并诱导炎症信号级联反应的细胞内阻断。在临床人群中,抗PC IgM水平升高与预防动脉粥样硬化相关,也可能下调自身免疫性疾病的严重程度。已分离出无高突变的人抗PC产生克隆,其同样能够区分凋亡细胞与健康细胞。一份关于无关成年人的独立报告描述了具有保守CDR3基序的IgM基因的抗PC产生B细胞,类似于B细胞慢性淋巴细胞白血病的定型克隆组。综上所述,新出现的证据表明,尽管人类免疫系统有能力形成实际上无限多样的Ig受体,但它可能经常反复产生表达具有保护和稳态作用的结构趋同的B细胞受体的淋巴细胞。

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