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Towards precision oncology in advanced prostate cancer

机译:在晚期前列腺癌中迈向精密肿瘤学

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Metastatic biopsy programmes combined with advances in genomic sequencing have provided new insights into the molecular landscape of castration-resistant prostate cancer (CRPC), identifying actionable targets, and emerging resistance mechanisms. The detection of DNA repair aberrations, such as mutation of BRCA2, could help select patients for poly(ADP-ribose) polymerase (PARP) inhibitor or platinum chemotherapy, and mismatch repair gene defects and microsatellite instability have been associated with responses to checkpoint inhibitor immunotherapy. Poor prognostic features, such as the presence of RB1 deletion, might help guide future therapeutic strategies. Our understanding of the molecular features of CRPC is now being translated into the clinic in the form of increased molecular testing for use of these agents and for clinical trial eligibility. Genomic testing offers opportunities for improving patient selection for systemic therapies and, ultimately, patient outcomes. However, challenges for precision oncology in advanced prostate cancer still remain, including the contribution of tumour heterogeneity, the timing and potential cooperation of multiple driver gene aberrations, and diverse resistant mechanisms. Defining the optimal use of molecular biomarkers in the clinic, including tissue-based and liquid biopsies, is a rapidly evolving field.
机译:转移活检程序与基因组测序的进展相结合,为抗阉割前列腺癌(CRPC)的分子景观提供了新的见解,鉴定了可操作的靶标和出现的抗性机制。 DNA修复像差的检测,例如BRCA2的突变,可以帮助为聚(ADP-核糖)聚合酶(PARP)抑制剂或铂化疗选择患者,并且错配修复基因缺陷和微卫星不稳定性与检查点抑制剂免疫疗法的反应有关。预后特征差,例如RB1删除的存在,可能有助于指导未来的治疗策略。我们对CRPC的分子特征的理解现在以增加的分子测试使用这些药剂和临床试验资格的形式转化为临床。基因组检测为改善全身疗法的患者选择提供了机会,最终患者结果。然而,晚期前列腺癌症精密肿瘤学的挑战仍然存在,包括肿瘤异质性,多种驾驶员基因畸变的时序和潜力合作以及多种抗性机制的贡献。定义临床中的分子生物标志物的最佳用途,包括组织基和液体活组织检查,是一种快速发展的田间。

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