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在一种新西兰混合(NZM)小鼠模型中,狼疮抗性与边缘区异常有关。

Lupus resistance is associated with marginal zone abnormalities in an NZM murine model.

作者信息

Duan Biyan, Croker Byron P, Morel Laurence

机构信息

Department of Pathology, Immunology and Laboratory Medicine, University of Florida College of Medicine, Gainesville, FL 32610-0275, USA.

出版信息

Lab Invest. 2007 Jan;87(1):14-28. doi: 10.1038/labinvest.3700497. Epub 2006 Nov 27.

Abstract

The NZM2410 and NZM TAN (TAN) are two of 27 inbred strains derived from an intercross between the NZW and NZB strains. NZM2410 mice develop a highly penetrant lupus nephritis mediated by three susceptibility loci, Sle1, Sle2 and Sle3. These three loci have been combined on a C57BL/6 background in a triple congenic strain that reconstitutes the NZM2410 autoimmune phenotype. Remarkably, inspite of the presence of Sle1, Sle2 and Sle3, TAN mice display a mild autoimmune phenotype reminiscent of NZW. Contrary to the lupus-prone strains, the majority of TAN CD4(+) T cells are in a naïve-inactivated stage. TAN mice show B-cell developmental abnormalities similar to lupus-prone mice, such an accumulation of transitional T1 cells and peritoneal B-1a cells. TAN mice show, however, a unique expansion of the splenic marginal zone, in which B cells express high levels of CD5 and CD9, fail to migrate to the follicles in response to LPS, and show sub-optimal binding of T-independent type 2 antigens. Therefore, TAN mice present a functional silencing of marginal zone B cells, which have been previously implicated with autoimmune process. The TAN strain thus provides a novel model for the analysis of the genetic determinants of B-cell autoreactivity.

摘要

NZM2410和NZM TAN(TAN)是从NZW和NZB品系杂交后代中衍生出的27个近交系中的两个。NZM2410小鼠会发展出一种由三个易感基因座Sle1、Sle2和Sle3介导的高渗透性狼疮性肾炎。这三个基因座已在C57BL/6背景上组合到一个三联同源近交系中,该品系重现了NZM2410自身免疫表型。值得注意的是,尽管存在Sle1、Sle2和Sle3,TAN小鼠却表现出一种类似于NZW的轻度自身免疫表型。与易患狼疮的品系相反,大多数TAN CD4(+) T细胞处于幼稚失活阶段。TAN小鼠表现出与易患狼疮小鼠相似的B细胞发育异常,如过渡性T1细胞和腹膜B-1a细胞的积累。然而,TAN小鼠的脾脏边缘区有独特的扩张,其中B细胞高水平表达CD5和CD9,对LPS无反应而无法迁移至滤泡,并显示对2型非依赖T细胞抗原的结合欠佳。因此,TAN小鼠呈现出边缘区B细胞的功能沉默,而边缘区B细胞此前被认为与自身免疫过程有关。TAN品系因此为分析B细胞自身反应性的遗传决定因素提供了一个新模型。

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