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Chemotherapy and immunotherapy combination in advanced prostate cancer

机译:化学疗法和免疫疗法联合治疗晚期前列腺癌

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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,有大量证据表明肿瘤从疾病的早期开始就促进了免疫耐受。通过抑制肿瘤并激活免疫系统的稳态机制,化学疗法可能有助于克服这种肿瘤诱导的免疫耐受性。因此,化学疗法因此可以支持新的免疫调节疗法的改善结果。前列腺癌特别适合于主动免疫疗法,因为前列腺肿瘤细胞表达许多独特的表面抗原。 Sipuleucel-T(最近在美国获得批准)是一种主动免疫疗法,可触发针对前列腺癌的T细胞反应。对III期试验参与者的一项探索性分析发现,在sipuleucel-T治疗几个月后,接受多西他赛治疗可显着提高生存率。然而,VITAL-2是一项III期临床试验,研究了前列腺癌治疗性疫苗加同时用多西紫杉醇与标准多西紫杉醇疗法在晚期前列腺癌中的关系,发现该疫苗方案总体存活率较低。该试验突出了与主动免疫疗法相比,关于化疗的最佳选择,剂量和时机的主要未解决问题。患者特征,前列腺癌疾病分期和治疗史也可能影响对联合治疗的反应。有效研究这些问题需要生物标志物验证和试验设计方面的进展。

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