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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >A New IRF-1-Driven Apoptotic Pathway Triggered by IL-4/IL-13 Kills Neonatal Th1 Cells and Weakens Protection against Viral Infection
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A New IRF-1-Driven Apoptotic Pathway Triggered by IL-4/IL-13 Kills Neonatal Th1 Cells and Weakens Protection against Viral Infection

机译:由IL-4 / IL-13引发的新的IRF-1驱动的凋亡途径杀死新生儿TH1细胞并削弱了对病毒感染的保护

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摘要

Early life immune responses are deficient in Th1 lymphocytes that compromise neonatal vaccination. We found that IL-4 and IL-13 engage a developmentally expressed IL-4R alpha/IL-13R alpha 1 heteroreceptor to endow IFN regulatory factor 1 (IRF-1) with apoptotic functions, which redirect murine neonatal Th1 reactivation to cell death. IL-4/IL-13-induced STAT6 phosphorylation serves to enhance IRF-1 transcription and promotes its egress from the nucleus. In the cytoplasm, IRF-1 can no longer serve as an anti-viral transcription factor but, instead, colocalizes with Bim and instigates the mitochondrial, or intrinsic, death pathway. The new pivotal function of IRF-1 in the death of neonatal Th1 cells stems from the ability of its gene to bind STAT6 for enhanced transcription and the proficiency of its protein to precipitate Bim-driven apoptosis. This cytokine-induced, IRF-1-mediated developmental death network weakens neonatal Th1 responses during early life vaccination and increases susceptibility to viral infection.
机译:早期生命免疫应答缺乏损害新生儿疫苗接种的淋巴细胞。我们发现IL-4和IL-13接合发育表达的IL-4Rα/ IL-13Rα1异质型以促进IFN调节因子1(IRF-1)与凋亡功能,将鼠新生儿TH1重新激活重新激活到细胞死亡中。 IL-4 / IL-13诱导的Stat6磷酸化用于增强IRF-1转录,并从细胞核中促进其出口。在细胞质中,IRF-1不能再用作抗病毒转录因子,而是用BIM结合,煽动线粒体或内在死亡途径。 IRF-1在新生儿TH1细胞死亡中的新枢轴功能源于其基因结合STAT6的能力,以增强转录和蛋白质的熟练程度,以沉淀BIM驱动的细胞凋亡。这种细胞因子诱导的IRF-1介导的发育死亡网络在早期植击期间削弱新生儿TH1反应,并增加了对病毒感染的敏感性。

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