首页> 外文期刊>Blood: The Journal of the American Society of Hematology >LMP1 signaling can replace CD40 signaling in B cells in vivo and has unique features of inducing class-switch recombination to IgG1.
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LMP1 signaling can replace CD40 signaling in B cells in vivo and has unique features of inducing class-switch recombination to IgG1.

机译:LMP1信号传导可以替代B细胞在体内的CD40信号传导,并具有诱导类开关重组为IgG1的独特功能。

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摘要

The Epstein-Barr virus (EBV) protein LMP1 is considered to be a functional homologue of the CD40 receptor. However, in contrast to the latter, LMP1 is a constitutively active signaling molecule. To compare B cell-specific LMP1 and CD40 signaling in an unambiguous manner, we generated transgenic mice conditionally expressing a CD40/LMP1 fusion protein, which retained the LMP1 cytoplasmic tail but has lost the constitutive activity of LMP1 and needs to be activated by the CD40 ligand. We show that LMP1 signaling can completely substitute CD40 signaling in B cells, leading to normal B-cell development, activation, and immune responses including class-switch recombination, germinal center formation, and somatic hypermutation. In addition, the LMP1-signaling domain has a unique property in that it can induce class-switch recombination to IgG1 independent of cytokines. Thus, our data indicate that LMP1 has evolved to imitate T-helper cell function allowing activation, proliferation, and differentiation of EBV-infected B cells independent of T cells.
机译:爱泼斯坦巴尔病毒(EBV)蛋白LMP1被认为是CD40受体的功能同源物。但是,与后者相反,LMP1是组成型活性信号分子。为了明确地比较B细胞特异性LMP1和CD40信号传导,我们产生了有条件表达CD40 / LMP1融合蛋白的转基因小鼠,该蛋白保留了LMP1的胞质尾巴,但失去了LMP1的组成活性,需要被CD40激活配体。我们显示,LMP1信号传导可以完全替代B细胞中的CD40信号传导,从而导致正常的B细胞发育,激活和免疫应答,包括类别开关重组,生发中心形成和体细胞超突变。此外,LMP1信号结构域具有独特的特性,因为它可以诱导类别转换重组为独立于细胞因子的IgG1。因此,我们的数据表明LMP1已进化为模仿T辅助细胞功能,从而可以独立于T细胞而激活,增殖和分化EBV感染的B细胞。

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