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Germinal Center Initiation, Variable Gene Region Hypermutation, and Mutant B Cell Selection without Detectable Immune Complexes on Follicular Dendritic Cells

机译:卵泡树突状细胞上的生发中心起始,可变基因区超突变和突变B细胞选择而无可检测的免疫复合物

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摘要

Serum antibody (Ab) can play several roles during B cell immune responses. Among these is to promote the deposition of immune complexes (ICs) on follicular dendritic cells (FDCs). ICs on FDCs are generally thought to be critical for normal germinal center (GC) formation and the development and selection of memory B cells. However, it has been very difficult to test these ideas. To determine directly whether FDC-bound complexes do indeed function in these roles, we have developed a transgenic (Tg) mouse in which all B lymphocytes produce only the membrane-bound form of immunoglobulin M. Immune Tg mice have 10,000-fold less specific Ab than wild-type mice and lack detectable ICs on FDCs. Nonetheless, primary immune responses and the GC reaction in these mice are robust, suggesting that ICs on FDCs do not play critical roles in immune response initiation and GC formation. Moreover, as indicated by the presence and pattern of somatic mutations, memory cell formation and selection appear normal in these IC-deficient GCs.
机译:血清抗体(Ab)在B细胞免疫反应中可以发挥多种作用。其中之一是促进免疫复合物(ICs)在滤泡树突状细胞(FDCs)上的沉积。通常认为FDC上的IC对正常生发中心(GC)的形成以及记忆B细胞的发育和选择至关重要。但是,很难测试这些想法。为了直接确定FDC结合的复合物是否确实发挥了这些作用,我们开发了一种转基因(Tg)小鼠,其中所有B淋巴细胞仅产生膜结合形式的免疫球蛋白M。免疫Tg小鼠的特异性抗体少10,000倍与野生型小鼠相比,FDC缺乏可检测的IC。尽管如此,这些小鼠的初次免疫反应和GC反应仍然很强健,这表明FDC上的IC在免疫反应的启动和GC形成中不发挥关键作用。而且,正如体细胞突变的存在和模式所表明的那样,在这些缺乏IC的GC中,记忆细胞的形成和选择似乎是正常的。

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