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Preserving genome integrity in human cells via DNA double-strand break repair

机译:通过DNA双链休息修复在人体细胞中保留基因组完整性

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摘要

The efficient maintenance of genome integrity in the face of cellular stress is vital to protect against human diseases such as cancer. DNA replication, chromatin dynamics, cellular signaling, nuclear architecture, cell cycle checkpoints, and other cellular activities contribute to the delicate spatiotemporal control that cells utilize to regulate and maintain genome stability. This perspective will highlight DNA double-strand break (DSB) repair pathways in human cells, how DNA repair failures can lead to human disease, and how PARP inhibitors have emerged as a novel clinical therapy to treat homologous recombination-deficient tumors. We briefly discuss how failures in DNA repair produce a permissive genetic environment in which preneoplastic cells evolve to reach their full tumorigenic potential. Finally, we conclude that an in-depth understanding of DNA DSB repair pathways in human cells will lead to novel therapeutic strategies to treat cancer and potentially other human diseases.
机译:在细胞应激面前的基因组完整性的有效维持至关重要,可防止癌症如癌症。 DNA复制,染色质动力学,蜂窝信号传导,核建筑,细胞周期检查点和其他细胞活性有助于细胞利用调节和维持基因组稳定性的微妙时尚控制。 这种观点将突出人体细胞中的DNA双链断裂(DSB)修复途径,DNA修复失败如何导致人类疾病,以及PARP抑制剂如何成为一种新的临床治疗以治疗同源重组缺陷型肿瘤。 我们简要讨论DNA修复的故障如何产生允许遗传环境,其中促塑料细胞进化以达到其全瘤瘤潜力。 最后,我们得出结论,对人体细胞中DNA DNA修复途径的深入了解将导致治疗癌症和潜在的其他人类疾病的新的治疗策略。

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