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Inhibition of DNA Repair in Cancer Therapy: Toward a Multi-Target Approach

机译:DNA修复在癌症治疗中的抑制作用:朝向多目标方法

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摘要

Alterations in DNA repair pathways are one of the main drivers of cancer insurgence. Nevertheless, cancer cells are more susceptible to DNA damage than normal cells and they rely on specific functional repair pathways to survive. Thanks to advances in genome sequencing, we now have a better idea of which genes are mutated in specific cancers and this prompted the development of inhibitors targeting DNA repair players involved in pathways essential for cancer cells survival. Currently, the pivotal concept is that combining the inhibition of mechanisms on which cancer cells viability depends is the most promising way to treat tumorigenesis. Numerous inhibitors have been developed and for many of them, efficacy has been demonstrated either alone or in combination with chemo or radiotherapy. In this review, we will analyze the principal pathways involved in cell cycle checkpoint and DNA repair focusing on how their alterations could predispose to cancer, then we will explore the inhibitors developed or in development specifically targeting different proteins involved in each pathway, underscoring the rationale behind their usage and how their combination and/or exploitation as adjuvants to classic therapies could help in patients clinical outcome.
机译:DNA修复途径的改变是癌症叛乱的主要驱动因素之一。然而,癌细胞比正常细胞更容易DNA损伤更容易受到DNA损伤,并且它们依赖于特定的功能修复途径以存活。由于基因组测序的进展,我们现在更好地了解哪些基因在特异性癌症中突变,并且这促使靶向DNA修复球员患者参与癌细胞生存至关重要的途径的抑制剂的发展。目前,关键概念是结合抑制癌细胞活力取决于治疗肿瘤鉴定最有希望的方法。已经开发了许多抑制剂,对于其中许多,已经单独或与化疗或放射疗法组合证明了功效。在这篇综述中,我们将分析细胞周期检查点和DNA修复所涉及的主要途径,重点关注其改变如何倾向于癌症,然后我们将探讨开发或开发的抑制剂,特别是针对每个途径所涉及的不同蛋白质,强调理论他们的使用背后以及他们的组合和/或剥削如何作为经典疗法的辅助剂可以帮助患者临床结果。

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