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Prostate cancer immunotherapy particularly in combination with androgen deprivation or radiation treatment. Customized pharmacogenomic approaches to overcome immunotherapy cancer resistance

机译:前列腺癌免疫疗法特别是与雄激素剥夺或放射治疗相结合。定制的药物基因组学方法可克服免疫疗法对癌症的抵抗力

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摘要

Conventional therapeutic approaches for advanced prostate cancer - such as androgen deprivation, chemotherapy, radiation - come up often against lack of effectiveness because of possible arising of correlative cancer cell resistance and/or inadequate anti-tumor immune conditions. Whence the timeliness of resorting to immune-based treatment strategies including either therapeutic vaccination-based active immunotherapy or anti-tumor monoclonal antibody-mediated passive immunotherapy. Particularly attractive, as for research studies and clinical applications, results to be the cytotoxic T-lymphocyte check point blockade by the use of anti-CTLA-4 and PD-1 monoclonal antibodies, particularly when combined with androgen deprivation therapy or radiation. Unlike afore said immune check point inhibitors, both cell-based (by the use of prostate specific antigen carriers autologous dendritic cells or even whole cancer cells) and recombinant viral vector vaccines are able to induce immune-mediated focused killing of specific antigen-presenting prostate cancer cells. Such vaccines, either used alone or concurrently/sequentially combined with above-mentioned conventional therapies, led to generally reach, in the field of various clinical trials, reasonable results particularly as regards the patient’s overall survival. Adoptive trasferred T-cells, as adoptive T-cell passive immunotherapy, and monoclonal antibodies against specific antigen-endowed prostate cancer cells can improve immune micro-environmental conditions. On the basis of a preliminary survey about various immunotherapy strategies, are here also outlined their effects when combined with androgen deprivation therapy or radiation. What’s more, as regard the immune-based treatment effectiveness, it has to be pointed out that suitable personalized epigenetic/gene profile-achieved pharmacogenomic approaches to target identified gene aberrations, may lead to overcome – as well as for conventional therapies – possible prostate cancer resistance to immunotherapy.
机译:晚期前列腺癌的常规治疗方法,例如雄激素剥夺,化学疗法,放射治疗,常常由于缺乏相关的癌细胞耐药性和/或抗肿瘤免疫条件不足而常常缺乏疗效。适时诉诸基于免疫的治疗策略,包括基于治疗疫苗的主动免疫治疗或抗肿瘤单克隆抗体介导的被动免疫治疗。对于研究和临床应用而言,特别有吸引力的是通过使用抗CTLA-4和PD-1单克隆抗体来阻断细胞毒性T淋巴细胞检查点,尤其是与雄激素剥夺疗法或放射疗法结合使用时。与前述的免疫检查点抑制剂不同,基于细胞的(通过使用前列腺特异性抗原载体自体树突状细胞或什至是整个癌细胞)和重组病毒载体疫苗均能够诱导免疫介导的对特异性抗原呈递前列腺的集中杀伤癌细胞。此类疫苗单独使用或与上述常规疗法同时/依次使用可在各种临床试验领域中普遍取得合理的结果,尤其是在患者的总体存活率方面。过继转移的T细胞,作为过继T细胞的被动免疫疗法,以及针对特定抗原赋予的前列腺癌细胞的单克隆抗体,可以改善免疫微环境条件。在对各种免疫治疗策略的初步调查的基础上,此处还概述了与雄激素剥夺治疗或放疗相结合时的效果。此外,就基于免疫的治疗效果而言,必须指出的是,针对个性化表观遗传学/基因概况的药物基因组学方法可用于靶向已鉴定的基因畸变,这可能会克服(以及对于传统疗法而言)可能的前列腺癌对免疫疗法的抵抗力。

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