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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Beyond the concept of cold and hot tumors for the development of novel predictive biomarkers and the rational design of immunotherapy combination
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Beyond the concept of cold and hot tumors for the development of novel predictive biomarkers and the rational design of immunotherapy combination

机译:超越冷热肿瘤的概念,开发新型预测性生物标志物,合理设计免疫治疗组合

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摘要

Immunotherapy has revolutionized the management of cancers. At the end of 2018,1,716 clinical trials assessed regimen that combine program death-1 (PD-1)/program death ligand-1 (PD-L1) blockers with other cancer therapies (tyrosine kinase inhibitor, chemotherapy and radiotherapy). There is a contrast between these clinical dynamics and the difficulty of identifying biomarkers to better select patients that could benefit from immunotherapy. In this context, different tumor classifications have been proposed to try to better stratify patients. They rely on the characteristics of the tumor microenvironment and led first to divide them into hot and cold tumors. In this review, we aim to demonstrate the limitations of this classification focusing on the differential significance of subpopulations of intratumor CD8 + T cells. We also underline novel mechanisms of resistance to anti-PD-l/PD-Ll blockade, focusing on myeloid cells, hypoxia and tumor immunoediting under treatment. Understanding the mechanisms of resistance to immune-checkpoint inhibitor is indeed a powerful research driver that allows further identification of novel biomarkers, drug development and bring a rational to innovative therapeutic combinations.
机译:免疫疗法彻底改变了癌症的管理。截至 2018 年底,1,716 项临床试验评估了将程序死亡 1 (PD-1)/程序死亡配体 1 (PD-L1) 阻滞剂与其他癌症疗法(酪氨酸激酶抑制剂、化疗和放疗)相结合的方案。这些临床动态与识别生物标志物以更好地选择可能从免疫治疗中受益的患者的困难之间存在对比。在这种情况下,已经提出了不同的肿瘤分类,以试图更好地对患者进行分层。它们依赖于肿瘤微环境的特征,并首先将它们分为热肿瘤和冷肿瘤。在这篇综述中,我们旨在证明这种分类的局限性,重点是肿瘤内CD8 + T细胞亚群的差异意义。我们还强调了抗PD-l/PD-L阻断耐药的新机制,重点关注治疗中的髓系细胞、缺氧和肿瘤免疫编辑。了解免疫检查点抑制剂耐药的机制确实是一个强大的研究驱动力,可以进一步识别新的生物标志物、药物开发,并为创新的治疗组合带来合理的选择。

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