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放疗对肿瘤微环境的重编程:对放疗与免疫治疗联合应用的启示

Reprogramming the tumour microenvironment by radiotherapy: implications for radiotherapy and immunotherapy combinations.

作者信息

Colton Madyson, Cheadle Eleanor J, Honeychurch Jamie, Illidge Tim M

机构信息

Division of Cancer Sciences, Manchester Academic Health Science Centre, NIHR Biomedical Research Centre, University of Manchester, Manchester, UK.

The Christie NHS Foundation Trust, Manchester, UK.

出版信息

Radiat Oncol. 2020 Nov 4;15(1):254. doi: 10.1186/s13014-020-01678-1.

Abstract

Radiotherapy (RT) is a highly effective anti-cancer therapy delivered to around 50-60% of patients. It is part of therapy for around 40% of cancer patients who are cured of their disease. Until recently, the focus of this anti-tumour efficacy has been on the direct tumour cytotoxicity and RT-induced DNA damage. Recently, the immunomodulatory effects of RT on the tumour microenvironment have increasingly been recognized. There is now intense interest in potentially using RT to induce an anti-tumour immune response, which has led to rethinking into how the efficacy of RT could be further enhanced. Following the breakthrough of immune check point inhibitors (ICIs), a new era of immuno-oncology (IO) agents has emerged and established immunotherapy as a routine part of cancer treatment. Despite ICI improving outcomes in many cancer types, overall durable responses occur in only a minority of patients. The immunostimulatory effects of RT make combinations with ICI attractive to potentially amplify anti-tumour immunity resulting in increased tumour responses and improved outcomes. In contrast, tumours with profoundly immunosuppressive tumour microenvironments, dominated by myeloid-derived cell populations, remain a greater clinical challenge and RT may potentially further enhance the immunosuppression. To harness the full potential of RT and IO agent combinations, further insights are required to enhance our understanding of the role these immunosuppressive myeloid populations play, how RT influences these populations and how they may be therapeutically manipulated in combination with RT to improve outcomes further. These are exciting times with increasing numbers of IO targets being discovered and IO agents undergoing clinical evaluation. Multidisciplinary research collaborations will be required to establish the optimal parameters for delivering RT (target volume, dose and fractionation) in combination with IO agents, including scheduling to achieve maximal therapeutic efficacy.

摘要

放射治疗(RT)是一种高效的抗癌疗法,约50%-60%的患者会接受该治疗。它是约40%治愈疾病的癌症患者治疗方案的一部分。直到最近,这种抗肿瘤疗效的重点一直放在直接的肿瘤细胞毒性和放疗诱导的DNA损伤上。最近,放疗对肿瘤微环境的免疫调节作用越来越受到认可。目前人们对潜在地利用放疗诱导抗肿瘤免疫反应有着浓厚兴趣,这导致人们重新思考如何进一步提高放疗的疗效。随着免疫检查点抑制剂(ICIs)的突破,免疫肿瘤学(IO)药物的新时代已经出现,并将免疫疗法确立为癌症治疗的常规组成部分。尽管ICIs改善了许多癌症类型的治疗结果,但总体持久反应仅发生在少数患者中。放疗的免疫刺激作用使得与ICIs联合使用具有吸引力,有可能增强抗肿瘤免疫力,从而增加肿瘤反应并改善治疗结果。相比之下,以髓系来源细胞群体为主的具有深度免疫抑制肿瘤微环境的肿瘤,仍然是一个更大的临床挑战,放疗可能会进一步增强免疫抑制作用。为了充分发挥放疗和IO药物联合使用的潜力,需要进一步深入了解这些免疫抑制性髓系群体所起的作用、放疗如何影响这些群体,以及如何与放疗联合进行治疗性调控以进一步改善治疗结果。随着越来越多的IO靶点被发现以及IO药物正在进行临床评估,现在是令人兴奋的时期。需要开展多学科研究合作,以确定与IO药物联合使用时放疗的最佳参数(靶区体积、剂量和分割方式),包括确定实现最大治疗效果的给药方案。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cc36/7640712/6161a3a36ef6/13014_2020_1678_Fig1_HTML.jpg

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