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The host STING pathway at the interface of cancer and immunity

机译:癌症和免疫力交界处的宿主STING途径

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A major subset of human cancers shows evidence for spontaneous adaptive immunity, which is reflected by the presence of infiltrating CD8~(+) T cells specific for tumor antigens within the tumor microenvironment. This observation has raised the question of which innate immune sensing pathway might detect the presence of cancer and lead to a natural adaptive antitumor immune response in the absence of exogenous infectious pathogens. Evidence for a critical functional role for type I IFNs led to interrogation of candidate innate immune sensing pathways that might be triggered by tumor presence and induce type I IFN production. Such analyses have revealed a major role for the stimulator of IFN genes pathway (STING pathway), which senses cytosolic tumor–derived DNA within the cytosol of tumor-infiltrating DCs. Activation of this pathway is correlated with IFN-β production and induction of antitumor T cells. Based on the biology of this natural immune response, pharmacologic agonists of the STING pathway are being developed to augment and optimize STING activation as a cancer therapy. Intratumoral administration of STING agonists results in remarkable therapeutic activity in mouse models, and STING agonists are being carried forward into phase I clinical testing.
机译:人类癌症的主要子集显示出自发适应性免疫的证据,这反映在肿瘤微环境中存在对肿瘤抗原具有特异性的浸润性CD8〜(+)T细胞。这一发现提出了一个问题,即在没有外源性传染病原体的情况下,哪种先天免疫传感途径可能检测到癌症并导致自然的适应性抗肿瘤免疫应答。 I型干扰素的关键功能作用的证据导致了对候选先天免疫感应途径的询问,该途径可能由肿瘤的存在触发并诱导I型干扰素的产生。此类分析揭示了IFN基因途径(STING途径)刺激物的主要作用,该途径可检测肿瘤浸润DC胞质内的细胞浆肿瘤衍生DNA。该途径的激活与IFN-β的产生和抗肿瘤T细胞的诱导相关。基于这种自然免疫反应的生物学特性,正在开发STING途径的药理激动剂,以增强和优化STING激活作为一种癌症疗法。瘤内给予STING激动剂可在小鼠模型中产生显着的治疗活性,并且STING激动剂正在进入I期临床试验。

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