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Auto-antibody production and glomerulonephritis in congenic Slamf1−/− and Slamf2−/− B6.129 but not in Slamf1−/− and Slamf2−/− BALB/c.129 mice

机译:在Slamf1-/-和Slamf2​​-/-B6.129中但在Slamf1-/-和Slamf2​​-/-BALB / c.129小鼠中不产生自身抗体和肾小球肾炎

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摘要

Several genes in an interval of human and mouse chromosome 1 are associated with a predisposition for systemic lupus erythematosus. Congenic mouse strains that contain a 129-derived genomic segment, which is embedded in the B6 genome, develop lupus because of epistatic interactions between the 129-derived and B6 genes, e.g. in B6.129chr1b mice. If a gene that is located on chromosome 1 is altered through homologous recombination in 129-derived embryonic stem cells (ES cells) and if the resultant knockout mouse is backcrossed with B6, interpretation of the phenotype of the mutant mouse may be affected by epistatic interactions between the 129 and B6 genomes. Here, we report that knockout mice of two adjacent chromosome 1 genes, Slamf1−/− and Slamf2−/−, which were generated with the same 129-derived ES cell line, develop features of lupus, if backcrossed on to the B6 genetic background. By contrast, Slamf1−/− [BALB/c.129] and Slamf2−/− [BALB/c.129] do not develop disease. Surprisingly, Slamf1−/− [B6.129] mice develop both auto-antibodies and glomerulonephritis between 3 and 6 months of age, while disease fully develops in Slamf1−/− [B6.129] mice after 9–14 months. Functional analyses of CD4+ T cells reveals that Slamf2−/− T cells are resistant to tolerance induction in vivo. We conclude that the Slamf2−/− mutation may have a unique influence on T-cell tolerance and lupus.
机译:人和小鼠1号染色体间隔内的几个基因与系统性红斑狼疮的易感性有关。由于129衍生基因和B6基因之间的上位性相互作用,包含嵌入到B6基因组中的包含129衍生基因组片段的同系小鼠品系发展为狼疮。在B6.129chr1b小鼠中。如果位于129号染色体的胚胎干细胞(ES细胞)中通过同源重组改变了位于1号染色体上的基因,并且如果所得的敲除小鼠与B6回交,那么上位相互作用可能会影响突变小鼠的表型解释在129和B6基因组之间。在这里,我们报道了敲除小鼠的两个相邻的1号染色体基因Slamf1 -/-和Slamf2​​ -/-,它们是用相同的129源ES细胞系生成的,如果回交到B6遗传背景,就会发展出狼疮的特征。相反,Slamf1 -/- [BALB / c.129]和Slamf2​​ -/- [BALB / c.129]没有发生疾病。出乎意料的是,Slamf1 -/- [B6.129]小鼠在3至6个月大时会同时出现自身抗体和肾小球肾炎,而疾病完全在 Slamf1 -/-< / sup> [B6.129] 小鼠9-14个月后。 CD4 + T细胞的功能分析表明, Slamf2​​ -/- T细胞对体内耐受诱导 具有抗性。我们得出结论, Slamf2​​ -// 突变可能对T细胞耐受性和狼疮具有独特的影响。

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