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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Cutting Edge: The Histone Methyltransferase G9a Is Required for Silencing of Helper T Lineage-Associated Genes in Proliferating CD8 T Cells
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Cutting Edge: The Histone Methyltransferase G9a Is Required for Silencing of Helper T Lineage-Associated Genes in Proliferating CD8 T Cells

机译:切削刃:组蛋白甲基转移酶G9A是在增殖CD8 T细胞中沉默辅助T谱系相关基因的沉默

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摘要

Helper versus cytotoxic T lineage decision in the thymus has been studied as a model for silencing of alternative lineage genes. Although the transcription factor RUNX3 is required for the initiation of Cd4 silencing in developing CD8 T cells, it is unknown how silencing of Cd4 and other helper T lineage genes is maintained. We show that the histone methyltransferase G9a is necessary for silencing helper T lineage genes in proliferating mouse CD8 T cells. Despite normal initial Cd4 downregulation, G9a-deficient CD8 T cells derepress Cd4 and other helper lineage genes during repeated division in lymphopenia or in response to tumor Ag. However, G9a was dispensable for continued silencing of those genes in CD8 T cells that respond to infection by Listeria monocytogenes. These results demonstrate that G9a facilitates maintenance of cellular identity of CD8 T cells during cell division, which is further reinforced by inflammatory signals.
机译:辅助与细胞毒性T族在胸腺中的逻辑决定被研究作为沉默替代谱系基因的模型。 尽管在开发CD8 T细胞时,CD4沉默的开始需要转录因子RUNX3,但是未知CD4和其他辅助T谱系基因的沉默。 我们表明,组蛋白甲基转移酶G9a对于在增殖小鼠CD8 T细胞中沉默辅助T谱系基因是必需的。 尽管正常的初始CD4下调,G9A缺陷的CD8 T细胞DEREPRESS CD4和其他促使螺旋谱基因在淋巴细胞症的重复分裂期间或响应于肿瘤AG。 然而,G9A可分配用于继续沉默于CD8 T细胞中的那些基因,这些基因响应李斯特菌单核细胞增生的感染。 这些结果表明,G9A促进在细胞分裂期间维持CD8 T细胞的细胞同一性,这通过炎症信号进一步加强。

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