Chappell Craig P, Draves Kevin E, Clark Edward A
Department of Immunology, School of Medicine, University of Washington, Seattle, Washington, United States of America.
Department of Microbiology, School of Medicine, University of Washington, Seattle, Washington, United States of America.
PLoS One. 2017 Mar 27;12(3):e0174661. doi: 10.1371/journal.pone.0174661. eCollection 2017.
CD22 is a BCR co-receptor that regulates B cell signaling, proliferation and survival and is required for T cell-independent Ab responses. To investigate the role of CD22 during T cell-dependent (TD) Ab responses and memory B cell formation, we analyzed Ag-specific B cell responses generated by wild-type (WT) or CD22-/- B cells following immunization with a TD Ag. CD22-/- B cells mounted normal early Ab responses yet failed to generate either memory B cells or long-lived plasma cells, whereas WT B cells formed both populations. Surprisingly, B cell expansion and germinal center (GC) differentiation were comparable between WT and CD22-/- B cells. CD22-/- B cells, however, were significantly less capable of generating a population of CXCR4hiCD38hi GC B cells, which we propose represent memory B cell precursors within GCs. These results demonstrate a novel role for CD22 during TD humoral responses evident during primary GC formation and underscore that CD22 functions not only during B cell maturation but also during responses to both TD and T cell-independent antigens.
CD22是一种BCR共受体,可调节B细胞信号传导、增殖和存活,是T细胞非依赖性抗体反应所必需的。为了研究CD22在T细胞依赖性(TD)抗体反应和记忆B细胞形成过程中的作用,我们分析了用TD抗原免疫后野生型(WT)或CD22-/- B细胞产生的抗原特异性B细胞反应。CD22-/- B细胞产生了正常的早期抗体反应,但未能产生记忆B细胞或长寿浆细胞,而WT B细胞则形成了这两种细胞群。令人惊讶的是,WT和CD22-/- B细胞之间的B细胞扩增和生发中心(GC)分化相当。然而,CD22-/- B细胞产生CXCR4hiCD38hi GC B细胞群的能力明显较低,我们认为这些细胞代表GC内的记忆B细胞前体。这些结果证明了CD22在TD体液反应中的新作用,这在原发性GC形成过程中很明显,并强调CD22不仅在B细胞成熟过程中起作用,而且在对TD和T细胞非依赖性抗原的反应中也起作用。
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