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Trial watch: STING agonists in cancer therapy

机译:试验观察:癌症治疗中的刺痛剂

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Stimulator of interferon response cGAMP interactor 1 (STING1, best known as STING) is an endoplasmic reticulum-sessile protein that serves as a signaling hub, receiving input from several pattern recognition receptors, most of which sense ectopic DNA species in the cytosol. In particular, STING ensures the production of type I interferon (IFN) in response to invading DNA viruses, bacterial pathogens, as well as DNA leaking from mitochondria or the nucleus (e.g., in cells exposed to chemotherapy or radiotherapy). As a type I IFN is critical for the initiation of anticancer immune responses, the pharmaceutical industry has generated molecules that directly activate STING for use in oncological indications. Such STING agonists are being tested in clinical trials with the rationale of activating STING in tumor cells or tumor-infiltrating immune cells (including dendritic cells) to elicit immunostimulatory effects, alone or in combination with a range of established chemotherapeutic and immunotherapeutic regimens. In this Trial Watch, we discuss preclinical evidence and accumulating clinical experience shaping the design of Phase I and Phase II trials that evaluate the safety and preliminary efficacy of STING agonists in cancer patients. ?2020, ?2020 The Author(s). Published with license by Taylor & Francis Group, LLC.
机译:干扰素响应的刺激器CGAMP相互动器1(Sting1,最可称为刺痛)的是一种内质网 - 无梗死蛋白,其用作信号传导毂,从若干模式识别受体接收输入,大部分是胞质溶胶中的易感异位DNA物种。特别地,刺痛确保响应于入侵DNA病毒,细菌病原体以及从线粒体或细胞核(例如,暴露于化疗或放射疗法的细胞中的DNA(例如,在暴露于化学疗法或放射疗法的细胞中,确保生产I型干扰素(IFN)。作为I型IFN对于启动抗癌免疫反应至关重要,制药工业已经产生了直接激活STING用于肿瘤的分子的分子。在临床试验中进行这种刺痛剂在临床试验中进行测试,其基本原理激活肿瘤细胞或肿瘤浸润的免疫细胞(包括树突细胞)以引发免疫刺激作用,单独或与一系列建立的化学治疗和免疫治疗方案组合。在这次试验中,我们讨论临床前证据,积累塑造阶段I和II期试验的临床经验,评价癌症患者的刺痛剂的安全性和初步效果。 ?2020,?2020作者。泰勒和弗朗西斯集团,LLC发布牌照。

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