Prostate Cancer and DNA Genes Repair: What Should an Oncologist Know? – A Narrative Review

Fernando Santos de Azevedo, Lanúscia Morais de Santana Sá, Uirá Maíra de Resende, Augusto Ribeiro Gabriel, Elisângela de Paula Silveira Lacerda
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Abstract

Prostate cancer is a very prevalent disease in men, especially in Western countries. The treatment of this neoplasm, both localized and locally advanced, is based on the clinical risk analysis (Gleason, tumor size, PSA, and other factors) and is founded on surgery and/or radiotherapy with or without androgen blockade with a GnRH analog (hormone gonadotropin releaser). However, in patients who invariably progress to a metastatic disease scenario, the tumors may present a heterogeneous behavior, depending on whether or not they are sensitive to androgen blockade therapy. Due to the poor prognosis of the metastatic castration-resistant scenario, current research carried out in the molecular biology and genetics field has identified several gene alterations associated with the development of prostate cancer, which correlate with clinical risk, therapeutic predictive responses, and prognosis. Among the associated gene alterations, the genes of the DNA repair pathway are correlated with diseases that present: a higher risk of recurrence; early metastasis; worse cancer-specific survival; familial risk, and predictive responses to new targeted therapies. Therefore, the breast cancer susceptibility genes, BRCA1 and BRCA2 (and other variants), present in the DNA repair machinery are being investigated to provide more (and better) therapeutic options for the treatment of the disease in the advanced scenario. This review was aimed to describe the malignant prostate disease, especially with regard to DNA repair mechanisms, genomic analysis of prostate cancer, predictive and prognostic implications, as well as on the development of poly-(ADP-ribose) polymerase (PARP) inhibitors, synthetic lethality mechanisms, and BRCAness phenomenon.
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前列腺癌和DNA基因修复:肿瘤学家应该知道什么?-叙事性回顾
前列腺癌是一种非常普遍的男性疾病,尤其是在西方国家。这种肿瘤的治疗,无论是局部还是局部晚期,都是基于临床风险分析(Gleason、肿瘤大小、PSA和其他因素),并建立在手术和/或放疗的基础上,有或没有GnRH类似物(激素促性腺激素释放剂)的雄激素阻断。然而,在总是进展为转移性疾病的患者中,肿瘤可能表现出异质行为,这取决于它们是否对雄激素阻断治疗敏感。由于转移性去势抵抗的预后较差,目前在分子生物学和遗传学领域开展的研究已经确定了几种与前列腺癌发展相关的基因改变,这些基因改变与临床风险、治疗预测反应和预后相关。在相关的基因改变中,DNA修复途径的基因与以下疾病相关:复发风险较高;早期的转移;更差的癌症特异性生存率;家族风险,以及对新靶向治疗的预测反应。因此,研究人员正在研究DNA修复机制中存在的乳腺癌易感基因BRCA1和BRCA2(以及其他变体),以便为晚期乳腺癌的治疗提供更多(更好)的治疗选择。本文综述了恶性前列腺疾病,特别是DNA修复机制、前列腺癌的基因组分析、预测和预后意义,以及聚(adp -核糖)聚合酶(PARP)抑制剂的开发、合成致死性机制和BRCAness现象。
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