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Parp inhibitors: An interesting pathway also for non-small cell lung cancer?

机译:Parp抑制剂:非小细胞肺癌的一条有趣途径也是吗?

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摘要

Treatment of lung cancer is improving, also based on the identification of molecular characteristics of the tumor, of which some already constitute promising targets. One of the molecular characteristics thought to play an important role in lung cancer is DNA repair dysfunctionality. Deregulated expression of DNA repair proteins, such as PARP, has been studied in lung cancer as a possible biomarker and clinically useful target, but the literature remains relatively poor. Pharmacological inactivation of PARP has allowed the identification of a synthetic lethality with a second DNA repair protein such as BRCA1, but has also shown the potential to sensitize tumors to commonly used cytotoxic agents. The current manuscript reviews data regarding PARP in the context of DNA repair and its different pathways, as well as the clinical data generated until now with PARP inhibitors. A deeper understanding of the DNA damage response in lung malignancies, and particularly a clarification of the crosstalk between DNA repair functionality and genetic stability, is the key to optimize the development of PARP inhibitors in the setting of NSCLC.
机译:肺癌的治疗也在改善,这也基于对肿瘤分子特征的鉴定,其中一些已经构成了有希望的靶标。被认为在肺癌中起重要作用的分子特征之一是DNA修复功能障碍。 DNA修复蛋白(例如PARP)的表达失调已在肺癌中进行了研究,作为可能的生物标志物和临床上有用的靶标,但相关文献仍然较少。 PARP的药理失活可以鉴定出具有第二种DNA修复蛋白(例如BRCA1)的合成致死性,但也显示出了使肿瘤对常用细胞毒剂敏感的潜力。本手稿回顾了有关DNA修复及其不同途径中PARP的数据,以及迄今为止使用PARP抑制剂产生的临床数据。深入了解肺恶性肿瘤中的DNA损伤反应,尤其是弄清DNA修复功能与遗传稳定性之间的串扰,是在NSCLC背景下优化PARP抑制剂开发的关键。

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