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首页> 外文期刊>The journal of immunology >Cutting Edge: Activation of STING in T Cells Induces Type I IFN Responses and Cell Death
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Cutting Edge: Activation of STING in T Cells Induces Type I IFN Responses and Cell Death

机译:前沿:T细胞中STING的激活诱导I型IFN反应和细胞死亡

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Stimulator of interferon genes (STING) was initially described as a sensor of intracellular bacterial and viral DNA and a promising adjuvant target in innate immune cells; more recently STING has also been shown to detect endogenous DNA and play a role in tumor immunity and autoimmune disease development. Thus far STING has been studied in macrophages and dendritic cells. In this study, to our knowledge we provide the first evidence of STING activation in T cells, in which STING agonists not only provoke type I IFN production and IFN-stimulated gene expression, mirroring the response of innate cells, but are also capable of activating cell stress and death pathways. Our results suggest a re-evaluation of STING agonist–based therapies may be necessary to identify the possible effects on the T cell compartment. Conversely, the effects of STING on T cells could potentially be harnessed for therapeutic applications.
机译:干扰素基因刺激物(STING)最初被描述为细胞内细菌和病毒DNA的传感器,也是先天免疫细胞中有希望的佐剂靶标。最近,STING也被证明可以检测内源性DNA,并在肿瘤免疫和自身免疫性疾病的发展中起作用。迄今为止,已经在巨噬细胞和树突状细胞中研究了STING。在这项研究中,据我们所知,我们提供了T细胞中STING活化的第一个证据,其中STING激动剂不仅激发I型IFN的产生和IFN刺激的基因表达,反映了先天细胞的反应,还能够活化细胞应激和死亡途径。我们的结果表明,可能需要对基于STING激动剂的疗法进行重新评估,以确定对T细胞区室的可能影响。相反,STING对T细胞的作用可潜在地用于治疗应用。

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