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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >AID constrains germinal center size by rendering B cells susceptible to apoptosis.
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AID constrains germinal center size by rendering B cells susceptible to apoptosis.

机译:AID通过使B细胞易于凋亡来限制生发中心的大小。

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摘要

The germinal center (GC) is a transient lymphoid tissue microenvironment that fosters T cell-dependent humoral immunity. Within the GC, the B cell-specific enzyme, activation-induced cytidine deaminase (AID), mutates the immunoglobulin locus, thereby altering binding affinity for antigen. In the absence of AID, larger GC structures are observed in both humans and mice, but the reason for this phenomenon is unclear. Because significant apoptosis occurs within the GC niche to cull cells that have acquired nonproductive mutations, we have examined whether a defect in apoptosis could account for the larger GC structures in the absence of AID. In this report, we reveal significantly reduced death of B cells in AID(-/-) mice as well as in B cells derived from AID(-/-) bone marrow in mixed bone marrow chimeric mice. Furthermore, AID-expressing B cells show decreased proliferation and survival compared with AID(-/-) B cells, indicating an AID-mediated effect on cellular viability. The GC is an etiologic site for B-cell autoimmunity and lymphomagenesis, both of which have been linked to aberrant AID activity. We report a link between AID-induced DNA damage and B-cell apoptosis that has implications for the development of B-cell disorders.
机译:生发中心(GC)是一种短暂的淋巴样组织微环境,可促进依赖T细胞的体液免疫。在GC中,B细胞特异性酶(激活诱导的胞苷脱氨酶(AID))使免疫球蛋白基因座突变,从而改变了对抗原的结合亲和力。在没有AID的情况下,在人和小鼠中均观察到较大的GC结构,但尚不清楚该现象的原因。由于GC生态位内发生了重要的凋亡,导致已获得非生产性突变的剔除细胞死亡,因此我们检查了凋亡的缺陷是否可以在没有AID的情况下解释较大的GC结构。在此报告中,我们揭示了混合骨髓嵌合小鼠中AID(-/-)小鼠以及源自AID(-/-)骨髓的B细胞的B细胞死亡显着减少。此外,与AID(-/-)B细胞相比,表达AID的B细胞显示出降低的增殖和存活率,表明AID介导的对细胞活力的影响。 GC是B细胞自身免疫和淋巴瘤发生的病因部位,两者均与异常的AID活性有关。我们报告了AID诱导的DNA损伤与B细胞凋亡之间的联系,这对B细胞疾病的发展有影响。

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