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Targeting Poly (ADP) Ribose Polymerase I (PARP-1) and PARP-1 Interacting Proteins for Cancer Treatment.

机译:针对癌症的靶向聚(ADP)核糖聚合酶I(PARP-1)和PARP-1相互作用蛋白。

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摘要

Cancer is a disease of uncontrolled cellular proliferation. Chemotherapy and radiation therapy are the two main modalities for cancer treatment. However, some cancer types have been found to be refractory to these treatments. Additionally, certain chemicals that are used in clinical trials produce high cytotoxicity as a secondary effect. Hence, current research is focused on finding ways by which cancer cells can be specifically sensitized to apoptotic death with minimal or no secondary effects on normal healthy cells. Since the resistance of cancer cells to DNA damaging agents stems from the modulation of DNA repair pathways, pharmacological inhibition of these pathways has been emerging as an effective tool for cancer treatment. Inhibition of key proteins involved in the molecular cascade of DNA damage detection and repair such as poly (ADP) ribose polymerase I (PARP-1) and its interacting proteins [DNA dependent protein kinase (DNA-PK) and Cockayne syndrome group B (CSB)] has recently proven to be successful for the treatment of various types of cancer cells and tumor xenografts in vitro. This review summarizes some of the recent findings and the potential application of DNA repair inhibitors in cancer treatment.
机译:癌症是细胞增殖失控的疾病。化学疗法和放射疗法是癌症治疗的两种主要方式。但是,已发现某些癌症类型对这些治疗无效。另外,临床试验中使用的某些化学药品会产生高细胞毒性,这是次要作用。因此,当前的研究集中在寻找使癌细胞对凋亡死亡特别敏感的方法,而对正常健康细胞的继发作用很小或没有。由于癌细胞对DNA破坏剂的抗性源于DNA修复途径的调节,因此这些途径的药理学抑制作用已成为治疗癌症的有效工具。抑制参与DNA损伤检测和修复的分子级联反应的关键蛋白,例如聚(ADP)核糖聚合酶I(PARP-1)及其相互作用蛋白[DNA依赖性蛋白激酶(DNA-PK)和Cockayne综合征B组(CSB) )]最近被证明在体外可成功治疗各种类型的癌细胞和肿瘤异种移植物。这篇综述总结了一些最新发现以及DNA修复抑制剂在癌症治疗中的潜在应用。

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