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大鼠唾液腺显示出比回肠更有限的IgA库。

Rat salivary gland reveals a more restricted IgA repertoire than ileum.

作者信息

Stoel Maaike, Evenhuis Willem N H, Kroese Frans G M, Bos Nicolaas A

机构信息

Department of Cell Biology, Immunology Section, University Medical Center Groningen, University of Groningen, A. Deusinglaan 1, 9713 AV Groningen, The Netherlands.

出版信息

Mol Immunol. 2008 Feb;45(3):719-27. doi: 10.1016/j.molimm.2007.07.001. Epub 2007 Aug 10.

Abstract

Secretory IgA is the most abundantly produced Ig in different mucosal tissues, such as the gastrointestinal tract and the salivary glands. These mucosal tissues are considered to be part of the common mucosal immune system. The specificity and immunoglobulin (Ig) VH gene repertoire of the IgA producing cells of both tissues is still largely unknown. To investigate the diversity of the antibody repertoire of IgA producing cells at different mucosal effector sites, we analysed used Ig VH genes by H-CDR3 spectrotyping and VH gene sequencing of both ileum and salivary gland IgA producing cells of PVG rats. Both types of tissues showed a limited diversity for the two major VH gene families, J558 and PC7183. The salivary gland showed even less diversity than the ileum of the same rat. Cloning and sequencing of used IgA VH genes confirmed the very restricted usage of VH genes since multiple sets of clonally related sequences in both types of tissues were found. More clones were found in salivary gland than in ileum and both tissues did not have shared VDJ joining regions. IgA derived from salivary gland used germline or near germline VH genes, whereas the ileal VH genes contained more mutations. Furthermore, clonal evolution patterns from all analyzed VH gene sequences of the salivary gland IgA producing cells show mainly randomly acquired somatic mutations, in contrast to the clonal evolution patterns often observed as a consequence of affinity maturation in germinal center reactions in peripheral lymphoid organs and Peyer's patches. Our results imply that IgA producing cells in the salivary gland are neither induced at the same place nor selected in the same way as the IgA producing cells in the ileum. The function of the IgA secreted by salivary gland is very likely a first line of defense with (near) germline encoded IgA, whereas in the intestine the majority of utilized IgA VH genes show evidence of somatic hypermutation.

摘要

分泌型免疫球蛋白A(Secretory IgA)是在不同黏膜组织(如胃肠道和唾液腺)中产生量最为丰富的免疫球蛋白。这些黏膜组织被认为是共同黏膜免疫系统的一部分。这两种组织中产生IgA的细胞的特异性和免疫球蛋白(Ig)VH基因库在很大程度上仍然未知。为了研究不同黏膜效应部位产生IgA的细胞的抗体库多样性,我们通过H - CDR3光谱分型以及对PVG大鼠回肠和唾液腺产生IgA的细胞进行VH基因测序,分析了所使用的Ig VH基因。两种组织对于两个主要VH基因家族J558和PC7183都显示出有限的多样性。唾液腺的多样性甚至比同一只大鼠的回肠还要少。对所使用的IgA VH基因进行克隆和测序证实了VH基因的使用非常受限,因为在两种组织中都发现了多组克隆相关序列。在唾液腺中发现的克隆比在回肠中更多,并且两种组织没有共享的VDJ连接区域。源自唾液腺的IgA使用种系或接近种系的VH基因,而回肠的VH基因含有更多突变。此外,唾液腺产生IgA的细胞的所有分析VH基因序列的克隆进化模式主要显示为随机获得的体细胞突变,这与在外周淋巴器官和派尔集合淋巴结生发中心反应中由于亲和力成熟而经常观察到的克隆进化模式形成对比。我们的结果表明,唾液腺中产生IgA的细胞既不是在同一位置诱导产生的,也不是以与回肠中产生IgA的细胞相同的方式被选择的。唾液腺分泌的IgA的功能很可能是以(接近)种系编码的IgA作为第一道防线,而在肠道中,大多数被利用的IgA VH基因显示出体细胞超突变的证据。

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