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Blimp‐1 induces and Hobit maintains the cytotoxic mediator granzyme B in CD8 T?cells

机译:软式小型飞船1诱发和习惯保持细胞毒性中介granzyme CD8 T ?

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Abstract CD8 T?cells acquire cytotoxic molecules including granzyme B during effector differentiation. Both tissue‐resident memory CD8 T?cells (Trm) and circulating CD45RA + effector‐type T?cells (Temra) cells have the ability to retain granzyme B protein expression into the memory phase, but it is unclear how this persistence of cytolytic activity is regulated during steady state. Previously, we have described that the transcriptional regulators Hobit and Blimp‐1 have overlapping target genes that include granzyme B, but their impact on the regulation of cytotoxicity in Trm and Temra cells during homeostasis has remained unclear. We examined the expression regulation of Hobit and Blimp‐1 in murine and human CD8 T‐cells to determine their timeframe of activity. While Blimp‐1 mRNA was expressed throughout effector and memory T?cells, Blimp‐1 protein, was only transiently expressed during the effector stage. In contrast, Hobit mRNA and protein expression was stably maintained during quiescence, but downregulated after activation. Notably, Blimp‐1 was required for expression of granzyme B in murine effector T?cells and Trm, while Hobit specifically regulated granzyme B in murine Trm during the memory phase. These findings suggest that Blimp‐1 initiates cytotoxic effector function and that Hobit maintains cytotoxicity in a deployment‐ready modus in Trm.
机译:抽象的CD8 T ?在效应包括granzyme B分化。T ?效应量类型T ?保留granzyme B蛋白表达的能力记忆阶段,但目前尚不清楚如何持久性的溶细胞的活动的监管在稳定状态。描述的转录监管机构习惯和顽固的1有重叠的目标基因包括granzyme B,但是他们的影响监管Trm Temra细胞的细胞毒性在体内平衡仍不清楚。检查表达式的习惯和监管软式小型飞船量1在小鼠和人类CD8 T细胞确定活动的时间。软式小型飞船在效应量1 mRNA表达和记忆T ?暂时性的表达效应阶段。相比之下,习惯mRNA和蛋白表达期间稳定保持静止,但激活后表达下调。所需granzyme B的表达吗小鼠效应T ?特别是在小鼠Trm granzyme B的管理在记忆阶段。软式小型飞船还是1启动细胞毒性效应功能和习惯保持细胞毒性一个部署准备测试请求信息的方法。

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