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IgM 和 IgM 记忆 B 细胞代表异质性群体,能够在再次受到疟原虫感染时产生类别转换抗体和生发中心 B 细胞。

IgM and IgM memory B cells represent heterogeneous populations capable of producing class-switched antibodies and germinal center B cells upon rechallenge with P. yoelii.

机构信息

Department of Microbiology and Immunology, University of Arkansas for Medical Sciences, Little Rock, Arkansas, USA.

出版信息

J Leukoc Biol. 2022 Nov;112(5):1115-1135. doi: 10.1002/JLB.4A0921-523R. Epub 2022 Jun 3.

Abstract

Memory B cells (MBCs) are essential for maintaining long-term humoral immunity to infectious organisms, including Plasmodium. MBCs are a heterogeneous population whose function can be dictated by isotype or expression of particular surface proteins. Here, aided by antigen-specific B-cell tetramers, MBC populations were evaluated to discern their phenotype and function in response to infection with a nonlethal strain of P. yoelii. Infection of mice with P. yoelii 17X resulted in 2 predominant MBC populations: somatically hypermutated isotype-switched (IgM ) and IgM MBCs that coexpressed CD73 and CD80 that produced antigen-specific antibodies in response to secondary infection. Rechallenge experiments indicated that IgG-producing cells dominated the recall response over the induction of IgM-secreting cells, with both populations expanding with similar timing during the secondary response. Furthermore, using ZsGreen1 expression as a surrogate for activation-induced cytidine deaminase expression alongside CD73 and CD80 coexpression, ZsGreen1 CD73 CD80 IgM , and IgM MBCs gave rise to plasmablasts that secreted Ag-specific Abs after adoptive transfer and infection with P. yoelii. Moreover, ZsGreen1 CD73 CD80 IgM and IgM MBCs could differentiate into B cells with a germinal center phenotype after adoptive transfer. A third population of B cells (ZsGreen1 CD73 CD80 IgM ) that is apparent after infection responded poorly to reactivation in vitro and in vivo, indicating that these cells do not represent a canonical population of MBCs. Together these data indicated that MBC function is not defined by immunoglobulin isotype, nor does coexpression of key surface markers limit the potential fate of MBCs after recall.

摘要

记忆 B 细胞(MBC)对于维持对感染病原体(包括疟原虫)的长期体液免疫至关重要。MBC 是一个异质性群体,其功能可以由同种型或特定表面蛋白的表达决定。在这里,借助抗原特异性 B 细胞四聚体,评估了 MBC 群体,以辨别它们在感染非致死性疟原虫株时的表型和功能。用疟原虫 17X 感染小鼠导致 2 种主要的 MBC 群体:体细胞超突变同种型转换(IgM)和 IgM MBC,它们共同表达 CD73 和 CD80,在二次感染时产生针对抗原的特异性抗体。再挑战实验表明,IgG 产生细胞在诱导 IgM 分泌细胞方面占主导地位,这两种群体在二次反应中以相似的时间扩展。此外,使用 ZsGreen1 表达作为激活诱导胞苷脱氨酶表达的替代物,与 CD73 和 CD80 共表达,ZsGreen1 CD73 CD80 IgM 和 IgM MBC 产生浆母细胞,在过继转移和感染疟原虫后分泌 Ag 特异性 Abs。此外,ZsGreen1 CD73 CD80 IgM 和 IgM MBC 可以在过继转移后分化为具有生发中心表型的 B 细胞。感染后出现的第三群 B 细胞(ZsGreen1 CD73 CD80 IgM)对体外和体内再激活反应不佳,表明这些细胞不代表经典的 MBC 群体。这些数据表明,MBC 功能不是由免疫球蛋白同种型定义的,关键表面标记物的共表达也不会限制 MBC 再激活后的潜在命运。

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