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自然自身抗体在 MRL-lpr 小鼠中的表达可预防狼疮肾炎并提高存活率。

Expression of natural autoantibodies in MRL-lpr mice protects from lupus nephritis and improves survival.

机构信息

Department of Pathology, University of Maryland School of Medicine, Baltimore, MD 21201, USA.

出版信息

J Immunol. 2012 Apr 15;188(8):3628-38. doi: 10.4049/jimmunol.1102859. Epub 2012 Mar 9.

Abstract

Natural autoantibodies (NAA) and their associated B cells constitute a substantial proportion of the normal Ab and B cell repertoire. They often have weak reactivity toward a variety of self-Ags such as DNA, nucleoproteins, and phospholipids. It remains controversial whether NAA contribute to or protect from autoimmune diseases. Using site-directed transgenic (sd-tg) mice expressing a prototypic NAA, we investigated the effect of NAA and NAA-producing B cells in disease development in the autoimmune-prone MRL/MpJ-Fas(lpr) (MRL-lpr) mice. We found that the expression of NAA in MRL-lpr mice prevented proteinuria and reduced kidney immune complex formation. The mice had significantly improved survival. Administration of the IgM NAA to MRL-lpr mice also delayed the onset of nephritis. The sd-tg MRL-lpr mice had decreased levels of anti-dsDNA Abs, anti-Hep2 nuclear Abs, and anti-Sm/ribonucleoprotein Abs. There is a shift in the IgG subclass profile from IgG2a and IgG3 to IgG1 in the sd-tg MRL-lpr mice. The CD4(+) T cells from the sd-tg MRL-lpr mice had increased expression of the negative costimulatory molecule CTLA-4 and increased production of IL-10 as compared with those from the wild-type mice. Furthermore, the NAA B cells produced large amounts of IL-10 upon TLR stimulation. These results indicate that NAA and NAA-producing B cells play an important role in protection from lupus nephritis and suggest that the NAA B cells may have an immune regulatory function via the provision of IL-10.

摘要

天然自身抗体 (NAA) 及其相关的 B 细胞构成了正常 Ab 和 B 细胞库的重要组成部分。它们通常对各种自身抗原(如 DNA、核蛋白和磷脂)具有较弱的反应性。NAA 是否有助于或保护自身免疫性疾病仍然存在争议。使用表达典型 NAA 的定点转基因 (sd-tg) 小鼠,我们研究了 NAA 和产生 NAA 的 B 细胞在自身免疫易感性 MRL/MpJ-Fas(lpr) (MRL-lpr) 小鼠疾病发展中的作用。我们发现,MRL-lpr 小鼠中 NAA 的表达可防止蛋白尿并减少肾脏免疫复合物形成。这些小鼠的存活率显著提高。向 MRL-lpr 小鼠给予 IgM NAA 也可延迟肾炎的发作。sd-tg MRL-lpr 小鼠的抗 dsDNA Ab、抗 Hep2 核 Ab 和抗 Sm/核糖核蛋白 Ab 水平降低。在 sd-tg MRL-lpr 小鼠中,IgG 亚类谱从 IgG2a 和 IgG3 向 IgG1 转移。与野生型小鼠相比,sd-tg MRL-lpr 小鼠的 CD4(+) T 细胞中负共刺激分子 CTLA-4 的表达增加,IL-10 的产生增加。此外,NAA B 细胞在 TLR 刺激下产生大量的 IL-10。这些结果表明 NAA 和产生 NAA 的 B 细胞在保护狼疮肾炎方面发挥重要作用,并表明 NAA B 细胞可能通过提供 IL-10 发挥免疫调节功能。

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