缺乏T-bet和胚外中胚层决定蛋白的CD8 + T细胞对病毒感染的异常17型反应。
Anomalous type 17 response to viral infection by CD8+ T cells lacking T-bet and eomesodermin.
作者信息
Intlekofer Andrew M, Banerjee Arnob, Takemoto Naofumi, Gordon Scott M, Dejong Caitlin S, Shin Haina, Hunter Christopher A, Wherry E John, Lindsten Tullia, Reiner Steven L
机构信息
Abramson Family Cancer Research Institute, University of Pennsylvania, Philadelphia, PA 19104, USA.
出版信息
Science. 2008 Jul 18;321(5887):408-11. doi: 10.1126/science.1159806.
Abstract
When intracellular pathogens invade mammalian hosts, naïve CD8+ T cells differentiate into cytotoxic killers, which lyse infected target cells and secrete cytokines that activate intracellular microbicides. We show that CD8+ T cells deficient in the transcription factors T-bet and eomesodermin (Eomes) fail to differentiate into functional killers required for defense against lymphocytic choriomeningitis virus. Instead, virus-specific CD8+ T cells lacking both T-bet and Eomes differentiate into an interleukin-17-secreting lineage, reminiscent of the helper T cell fate that has been implicated in autoimmunity and extracellular microbial defense. Upon viral infection, mice with T cells lacking both T-bet and Eomes develop a CD8+ T cell-dependent, progressive inflammatory and wasting syndrome characterized by multi-organ infiltration of neutrophils. T-bet and Eomes, thus, ensure that CD8+ T cells adopt an appropriate course of intracellular rather than extracellular destruction.
摘要
当细胞内病原体侵入哺乳动物宿主时,初始CD8 + T细胞分化为细胞毒性杀伤细胞,后者裂解被感染的靶细胞并分泌激活细胞内杀菌剂的细胞因子。我们发现,缺乏转录因子T-bet和胚外中胚层决定蛋白(Eomes)的CD8 + T细胞无法分化为抵御淋巴细胞性脉络丛脑膜炎病毒所需的功能性杀伤细胞。相反,同时缺乏T-bet和Eomes的病毒特异性CD8 + T细胞分化为分泌白细胞介素-17的谱系,这让人联想到与自身免疫和细胞外微生物防御有关的辅助性T细胞命运。病毒感染后,同时缺乏T-bet和Eomes的T细胞的小鼠会出现一种依赖CD8 + T细胞的进行性炎症和消瘦综合征,其特征是中性粒细胞多器官浸润。因此,T-bet和Eomes确保CD8 + T细胞采取适当的细胞内而非细胞外破坏途径。
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