细胞外信号调节激酶2(Erk2)丝裂原活化蛋白激酶调节CD8 T细胞的增殖和存活。
The Erk2 MAPK regulates CD8 T cell proliferation and survival.
作者信息
D'Souza Warren N, Chang Chiung-Fang, Fischer April M, Li Manqing, Hedrick Stephen M
机构信息
Department of Cellular and Molecular Medicine, Division of Biological Science, Molecular Biology Section, University of California, San Diego, La Jolla, CA 92093, USA.
出版信息
J Immunol. 2008 Dec 1;181(11):7617-29. doi: 10.4049/jimmunol.181.11.7617.
Abstract
The magnitude of T cell responses is determined by proliferation and survival decisions made by the responding cells. We now demonstrate that the Erk MAPK pathway plays a critical role in these cell fate decisions within CD8 T cells. While Erk1 is dispensable for all aspects of CD8 T cell activation, Erk2 is required for the proliferation of CD8 T cells activated in the absence of costimulation. Surprisingly, Erk2 is not required for proliferation following the addition of a costimulatory signal in vitro, or upon viral infection in vivo, but regulates the size of the responding population by enhancing cell survival. An important component of this Erk2-derived signal is the transcriptional regulation of Bcl-2 family members Bcl-x(L) and Bim, and impaired Erk2-deficient CD8 T cell survival can be rescued by genetic ablation of Bim. These studies ascribe multifaceted functions specific to Erk2 in CD8 T cell activation, proliferation, and survival.
摘要
T细胞反应的强度由反应细胞做出的增殖和存活决定所决定。我们现在证明,Erk MAPK通路在CD8 T细胞内的这些细胞命运决定中起关键作用。虽然Erk1对于CD8 T细胞激活的所有方面都是可有可无的,但Erk2是在没有共刺激的情况下被激活的CD8 T细胞增殖所必需的。令人惊讶的是,在体外添加共刺激信号后或在体内病毒感染后,增殖并不需要Erk2,但它通过提高细胞存活率来调节反应群体的大小。这种源自Erk2的信号的一个重要组成部分是对Bcl-2家族成员Bcl-x(L)和Bim的转录调控,并且通过对Bim进行基因消融可以挽救Erk2缺陷型CD8 T细胞受损的存活率。这些研究揭示了Erk2在CD8 T细胞激活、增殖和存活中特有的多方面功能。
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