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Tumor and Host Factors Controlling Antitumor Immunity and Efficacy of Cancer Immunotherapy

机译:肿瘤和宿主因素控制抗肿瘤免疫和癌症免疫疗法的功效。

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Abstract Despite recent clinical advances in immunotherapy, a fraction of cancer patients fails to respond to these interventions. Evidence from preclinical mouse models as well as clinical samples has provided evidence that the extent of activated T cell infiltration within the tumor microenvironment is associated with clinical response to immunotherapies including checkpoint blockade. Therefore, understanding the molecular mechanisms mediating the lack of T cell infiltration into the tumor microenvironment will be instrumental for the development of new therapeutic strategies to render those patients immunotherapy responsive. Recent data have suggested that major sources of inter-subject heterogeneity include differences in somatic mutations in specific oncogene pathways between cancers of individual subjects and also environmental factors including commensal microbial composition. Successful identification of such causal factors should lead to new therapeutic approaches that may facilitate T cell entry into non-inflamed tumors and expand the fraction of patients capable of responding to novel immunotherapies.
机译:摘要尽管最近在免疫疗法方面取得了临床进展,但仍有一部分癌症患者对这些干预措施没有反应。来自临床前小鼠模型以及临床样品的证据提供了证据,即肿瘤微环境中活化的T细胞浸润的程度与对免疫疗法的临床反应(包括检查点封锁)相关。因此,了解介导缺乏T细胞浸润进入肿瘤微环境的分子机制将有助于开发新的治疗策略,使这些患者对免疫疗法具有响应性。最近的数据表明,受试者间异质性的主要来源包括个体受试者的癌症之间特定致癌基因途径中体细胞突变的差异,以及包括共生微生物组成在内的环境因素。成功鉴定出此类病因后,应会产生新的治疗方法,以促进T细胞进入非炎症性肿瘤并扩大能够对新型免疫疗法产生反应的患者比例。

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