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Chemotherapy and immunotherapy combination in advanced prostate cancer

机译:化疗和免疫治疗相结合晚期前列腺癌

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In prostate cancer, there is considerable evidence that tumors promote immune tolerance starting early in the disease. By suppressing tumors and activating immune system homeostatic mechanisms, chemotherapy may help overcome this tumor-induced immune tolerance. As such, chemotherapy may therefore support improved results from novel immune-modulating therapies. Prostate cancer is particularly suited for active immunotherapy because prostate tumor cells express a number of distinctive surface antigens. Sipuleucel-T, which has recently been approved in the United States, is an active immunotherapy that triggers T-cell responses against prostate cancer. An exploratory analysis of phase III trial participants found a substantial survival benefit to receiving docetaxel some months after sipuleucel-T. However, VITAL-2, a phase III trial investigating a prostate cancer therapeutic vaccine plus concurrent docetaxel versus standard docetaxel therapy in advanced prostate cancer, observed lower overall survival with the vaccine regimen. This trial highlights major unresolved questions concerning the optimum choice, dosing, and timing of chemotherapy relative to active immunotherapy. Patient characteristics, prostate cancer disease stage, and treatment history also may influence the response to combined therapy. Advances in biomarker validation and trial design are needed to efficiently investigate these issues.
机译:在前列腺癌中,有相当多的证据肿瘤促进免疫耐受开始在疾病的早期。激活免疫系统稳态机制,化疗可以帮助克服这个肿瘤导致免疫耐受。因此支持改善结果的小说immune-modulating疗法。特别适合主动免疫疗法因为前列腺肿瘤细胞表达的独特的表面抗原。最近在美国被批准,是一个活跃的触发t细胞免疫治疗对前列腺癌的反应。三期临床试验参与者的分析发现实质性的生存受益多烯紫杉醇sipuleucel-T后几个月。然而,VITAL-2,第三期临床试验研究前列腺癌治疗性疫苗+并发多烯紫杉醇和多烯紫杉醇标准治疗晚期前列腺癌,观察降低总体生存与疫苗疗法。这个试验突出了主要的未解决的问题关于最优选择、剂量和时间相对于主动免疫治疗的化疗。病人的特点,前列腺癌疾病阶段,历史也可能影响治疗的响应相结合治疗。生物标记验证和试验设计是必要的有效地研究这些问题。

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