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T 细胞非依赖型 IgA 类别转换重组仅限于 GALT 并发生在明显生发中心形成之前。

T cell-independent IgA class switch recombination is restricted to the GALT and occurs prior to manifest germinal center formation.

机构信息

Department of Microbiology and Immunology, Mucosal Immunobiology and Vaccine Center, Institute of Biomedicine, University of Gothenburg, Gothenburg, Sweden.

出版信息

J Immunol. 2010 Apr 1;184(7):3545-53. doi: 10.4049/jimmunol.0901895. Epub 2010 Mar 5.

Abstract

Recently, we reported that CD40(-/-) mice, exhibiting exclusively T cell-independent IgA class switch recombination (CSR), demonstrated near normal levels of IgA plasma cells in the gut lamina propria (LP), despite the complete lack of germinal centers (GCs). In this study, we have extended our analysis focusing on how to reconcile these findings using flow cytometry and molecular markers for IgA CSR. In agreement with our previous results with small intestinal LP, the colon LP was found to host IgA CSR only when lymphoid follicles were present. Thus, no IgA CSR was observed in the nonorganized colon LP. By contrast, the Peyer's patch (PP) was the dominant IgA CSR site in both CD40(-/-) and wild type (WT) mice, and they both hosted similar levels of mRNA expression for B cell activating factor of the TNF family, a proliferation inducing ligand, and inducible NO synthase, potential switch-factors for IgA. Unexpectedly, we found that PP B cells undergoing IgA CSR were GL7-intermediate. These cells had not undergone somatic hypermutations (SHMs), whereas GL7-high cells in WT PP, which exhibited GCs, were heavily mutated. Moreover, IgA plasma cells in the LP of CD40(-/-) mice demonstrated few mutations in their Ig V regions, whereas WT LP B cells from different sites showed extensive SHMs, which were also clonally related. Therefore, IgA CSR can occur in PP at a stage preceding manifest GC (GL7-intermediate), whereas SHM require GC formations (GL7-high). These findings reconcile that IgA CSR can occur in PP in the absence of GC with the fact that CD40(-/-) mice host near normal levels of IgA plasma cells in the LP.

摘要

最近,我们报道了 CD40(-/-) 小鼠仅表现出 T 细胞非依赖性 IgA 类别转换重组(CSR),尽管完全缺乏生发中心(GC),但其肠道固有层(LP)中的 IgA 浆细胞水平接近正常。在这项研究中,我们通过流式细胞术和 IgA CSR 的分子标记物,扩展了我们的分析,以研究如何调和这些发现。与我们之前在小肠 LP 中的结果一致,当存在淋巴滤泡时,结肠 LP 才会发生 IgA CSR。因此,在无组织的结肠 LP 中未观察到 IgA CSR。相比之下,派尔集合淋巴结(PP)是 CD40(-/-) 和野生型(WT)小鼠中 IgA CSR 的主要部位,并且它们都具有相似水平的 TNF 家族 B 细胞激活因子、增殖诱导配体和诱导型一氧化氮合酶的 mRNA 表达,这些都是 IgA 的潜在转换因子。出乎意料的是,我们发现正在经历 IgA CSR 的 PP B 细胞是 GL7 中间型。这些细胞未发生体细胞高突变(SHM),而 WT PP 中表现出 GC 的 GL7 高细胞则发生了大量突变。此外,CD40(-/-) 小鼠 LP 中的 IgA 浆细胞在其 Ig V 区中显示出很少的突变,而来自不同部位的 WT LP B 细胞则显示出广泛的 SHM,并且这些细胞还存在克隆相关。因此,IgA CSR 可以在 PP 中在明显 GC(GL7 中间型)之前的阶段发生,而 SHM 需要 GC 形成(GL7 高型)。这些发现调和了 IgA CSR 可以在没有 GC 的情况下在 PP 中发生的事实,即 CD40(-/-) 小鼠在 LP 中具有接近正常水平的 IgA 浆细胞。

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