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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >The T Cell-Dependent B Cell Immune Response and Germinal Center Reaction Are Intact in A-myb-Deficient Mice
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The T Cell-Dependent B Cell Immune Response and Germinal Center Reaction Are Intact in A-myb-Deficient Mice

机译:T细胞依赖性B细胞免疫反应和生殖中心反应在A-myb缺陷小鼠中完好无损。

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摘要

Expression of the protooncogene A-myb is restricted to the developing CNS, adult testes, breasts in late pregnancy, and genninal centers of secondary B cell follicles. The functional relevance of A-myb expression at three of these sites has been demonstrated previously via the generation and analysis of A-myb-deficient mice, which display behavioral abnormalities, male sterility, and perturbed breast development during pregnancy. In contrast, here we show that the germinal center response driven by T cell-dependent Ag immunization and the associated processes of Ab V gene somatic hypermutation, affinity maturation, and heavy chain class switching are overtly normal in A-myb-deficient mice. Nonetheless, these mice display mild splenic white pulp hypo oplasia and blunted primary serum Ab responses, suggesting that although A-myb is not directly involved in the regulation of the memory B cell response, it may playa role in enhancing peripheral B cell survival or proliferative capacity.
机译:原癌基因A-myb的表达仅限于发育中的中枢神经系统,成年睾丸,妊娠晚期的乳房以及继发性B细胞滤泡的生殖器中心。先前已通过A-myb缺陷小鼠的产生和分析证明了A-myb在这三个位点的表达在功能上的相关性,这些小鼠表现出行为异常,雄性不育和怀孕期间乳房发育受干扰。相比之下,在这里我们显示,在A-myb缺陷型小鼠中,由T细胞依赖性Ag免疫和Ab V基因体细胞超突变,亲和力成熟以及重链类别转换的相关过程驱动的生发中心反应明显是正常的。然而,这些小鼠表现出轻度的脾脏白浆膜轻视和原发性血清Ab反应减弱,表明尽管A-myb不直接参与记忆B细胞反应的调节,但可能在增强外周血B细胞存活或增殖中发挥作用容量。

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