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Lyn 信号转导上调 GANP 对于淋巴器官生发中心高亲和力 B 细胞的存活至关重要。

Lyn signaling to upregulate GANP is critical for the survival of high-affinity B cells in germinal centers of lymphoid organs.

机构信息

Department of Immunology, Graduate School of Medical Sciences, Kumamoto University, Kumamoto 860-8556, Japan.

出版信息

J Immunol. 2012 Oct 1;189(7):3472-9. doi: 10.4049/jimmunol.1200649. Epub 2012 Aug 31.

Abstract

Signals through BCR and costimulatory molecules play essential roles in selecting high-affinity B cells with Ig V-region mutations in the germinal centers (GCs) of peripheral lymphoid organs. Lyn-deficient (lyn(-/-)) mice show impaired BCR signal triggering for cell proliferation and GC formation, causing hyper-IgM, and display autoimmunity after aging. In this study, we demonstrate that Lyn-mediated signaling to upregulate GANP is essential for the survival of mature GC-like (mGC) B cells with high-affinity type BCR mutations upon Ag immunization. Transgenic ganp expression into lyn(-/-) mice did not recover the Lyn-deficient phenotype with regard to B cell differentiation, serum Igs, and impaired GC formation in spleens after immunization with nitrophenyl-chicken γ-globulin, but it markedly rescued cell survival of mGC B cells by suppressing DNA damage, thereby increasing the frequency of the Trp(33)-to-Leu mutation in the IgV(H)-186.2 region and affinity maturation of nitrophenyl-binding B cells. GANP may play a critical role in Lyn-mediated signaling for the selection of high-affinity B cells in peripheral lymphoid organs.

摘要

BCR 和共刺激分子信号在选择外周淋巴器官生发中心(GC)中具有 Ig V 区突变的高亲和力 B 细胞中发挥重要作用。Lyn 缺陷(lyn(-/-))小鼠显示 BCR 信号触发细胞增殖和 GC 形成受损,导致高 IgM,并在衰老后出现自身免疫。在这项研究中,我们证明了 Lyn 介导的信号转导上调 GANP 对于在抗原免疫后具有高亲和力 BCR 突变的成熟 GC 样(mGC)B 细胞的存活是必不可少的。将 ganp 转基因表达到 lyn(-/-)小鼠中并没有恢复 Lyn 缺陷表型,包括 B 细胞分化、血清 Ig 和用硝基苯鸡 γ-球蛋白免疫后脾脏中 GC 形成受损,但它通过抑制 DNA 损伤显著挽救了 mGC B 细胞的存活,从而增加了 IgV(H)-186.2 区域中 Trp(33)-to-Leu 突变的频率和硝基苯结合 B 细胞的亲和力成熟。GANP 可能在 Lyn 介导的外周淋巴器官中高亲和力 B 细胞选择的信号转导中发挥关键作用。

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