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Half of the T-cell repertoire combinatorial diversity is genetically determined in humans and humanized mice

机译:一半的t细胞剧目组合在人类和多样性是由基因决定的人性化的小鼠

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摘要

In humanized mice, the T-cell repertoire is derived from genetically identical human progenitors in distinct animals. Thus, careful comparison of the T-cell repertoires of humanized mice with those of humans may reveal the contribution of genetic determinism on T-cell repertoire formation. Here, we performed a comprehensive assessment of the distribution of V-J combinations of the human β chain of the T-cell receptor (hTRBV) in NOD.SCID.γc -/- (NSG) humanized mice. We observed that numerous V-J combinations were equally distributed in the thymus and in the periphery of humanized mice compared with human references. A global analysis of the data, comparing repertoire perturbation indices in humanized NSG mice and unrelated human PBMCs, reveals that 50% of the hTRBV families significantly overlapped. Using multivariate ranking and bootstrap analyses, we found that 18% of all possible V-J combinations contributed close to 50% of the expressed diversity, with significant over-representation of BV5-J1.1+1.2 and BV6-J1.1+1.2 rearrangements. Finally, comparison of CD3 - and CD3 + thymocyte repertoires indicated that the observed V-J combination overlap was already present before TCR-MHC selection in the thymus. Altogether, our results show that half of the T-cell repertoire combinatorial diversity in humans is genetically determined.
机译:人源化小鼠的t细胞剧目来自人类基因完全相同祖细胞在不同的动物。比较人性化的t细胞体验老鼠与人类可能揭示了在t细胞遗传决定论的贡献曲目的形成。分布的综合评估日本宣布投降的人类β链的组合在NOD.SCID t细胞受体(hTRBV)。人性化的老鼠。均匀分布的组合胸腺和人源化小鼠的外围相比之下,人类的引用。的数据,比较曲目扰动指数在人性化的NSG老鼠和人类无关PBMCs hTRBV显示,50%的家庭明显的重叠。排名和引导分析,我们发现,18%所有可能的胜利贡献组合近50%的多样性,表达BV5-J1.1 + 1.2的重要代表和BV6-J1.1 + 1.2重组。比较CD3 -和CD3 +胸腺细胞体验观察表明,v - j结合重叠之前就已经存在在胸腺TCR-MHC选择。结果表明,t细胞剧目的一半组合在人类基因多样性确定。

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