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Mechanistic Insights into Molecular Targeting and Combined Modality Therapy for Aggressive, Localized Prostate Cancer.

机译:分子靶向和联合模式治疗侵略性,局部前列腺癌的机制研究。

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摘要

Radiation therapy (RT) is one of the mainstay treatments for prostate cancer (PCa). The potentially curative approaches can provide satisfactory results for many patients with non-metastatic PCa; however, a considerable number of individuals may present disease recurrence and die from the disease. Exploiting the rich molecular biology of PCa will provide insights into how the most resistant tumor cells can be eradicated to improve treatment outcomes. Important for this biology-driven individualized treatment is a robust selection procedure. The development of predictive biomarkers for RT efficacy is therefore of utmost importance for a clinically exploitable strategy to achieve tumor-specific radiosensitization. This review highlights the current status and possible opportunities in the modulation of four key processes to enhance radiation response in PCa by targeting the: (1) androgen signaling pathway; (2) hypoxic tumor cells and regions; (3) DNA damage response (DDR) pathway; and (4) abnormal extra-/intracell signaling pathways. In addition, we discuss how and which patients should be selected for biomarker-based clinical trials exploiting and validating these targeted treatment strategies with precision RT to improve cure rates in non-indolent, localized PCa.
机译:放射疗法(RT)是前列腺癌(PCa)的主要疗法之一。潜在的治疗方法可以为许多非转移性PCa患者提供满意的结果。但是,相当多的人可能会复发并死于该疾病。利用PCa的丰富分子生物学将提供有关如何消除最耐药的肿瘤细胞以改善治疗效果的见解。对于这种由生物学驱动的个体化治疗,重要的是要有一个稳健的选择程序。因此,RT疗效预测性生物标志物的开发对于实现肿瘤特异性放射增敏的临床可利用策略至关重要。这篇综述着重于通过针对以下方面来增强PCa辐射响应的四个关键过程的调制的现状和可能的机会:(1)雄激素信号传导途径; (2)低氧肿瘤细胞和区域; (3)DNA损伤反应(DDR)途径; (4)细胞外/细胞内信号通路异常。此外,我们讨论了如何以及应该选择哪些患者进行基于生物标志物的临床试验,这些患者利用精确的RT来开发和验证这些靶向治疗策略,以提高非惰性局部PCa的治愈率。

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