首页> 外文期刊>Journal of Pharmacological and Toxicological Methods >Development of a high-throughput screening-amenable assay for human poly(ADP-ribose) polymerase inhibitors.
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Development of a high-throughput screening-amenable assay for human poly(ADP-ribose) polymerase inhibitors.

机译:高通量筛选适合人类聚(ADP-核糖)聚合酶抑制剂的测定方法的开发。

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INTRODUCTION: Poly(ADP-ribose) polymerase (PARP) plays a pivotal role in the repair of DNA strand breaks. However, excessive activation of PARP causes a rapid depletion of intracellular energy, leading to cell death. Inhibitors of PARP have been shown to reduce infarct size in animal models of myocardial ischemia. PARP inhibitors may have potential therapeutic benefit in the treatment of myocardial ischemia, stroke, head trauma, and neurodegenerative disease, and as an adjunct therapy with chemotherapeutic agents/radiation in cancer therapy. METHODS: Assays reported in the literature and commercially available PARP assay kits are labor-intensive, use radioactive reagents, use antibodies, and are not readily amenable to high throughput screening (HTS) [corrected]. Here we report the development and the validation of a nonradioactive PARP assay suitable for HTS. This is a biotinylated NAD-based colorimetric assay in a 96-well plate format. RESULTS: The assay is sensitive, reproducible, and easy to use. The IC(50) values generated for the known PARP inhibitors are in agreement with those generated using the commercial radioactive kit and those reported in the literature. DISCUSSION: The present study demonstrates a sensitive and reproducible methodology capable of screening human PARP inhibitors in high-throughput format.
机译:简介:聚(ADP-核糖)聚合酶(PARP)在修复DNA链断裂中起着关键作用。但是,PARP的过度激活会导致细胞内能量迅速耗尽,从而导致细胞死亡。在心肌缺血的动物模型中,PARP抑制剂可减少梗塞面积。 PARP抑制剂可能在治疗心肌缺血,中风,头部外伤和神经退行性疾病方面具有潜在的治疗优势,并且在癌症治疗中作为化学疗法/放射线的辅助疗法。方法:文献报道的测定法和可商购的PARP测定试剂盒费力,使用放射性试剂,使用抗体,并且不易接受高通量筛选(HTS)[校正]。在这里,我们报告适用于HTS的非放射性PARP分析的发展和验证。这是96孔板形式的基于生物素化NAD的比色测定。结果:该测定法灵敏,可重复且易于使用。对于已知的PARP抑制剂产生的IC(50)值与使用商业放射性试剂盒产生的IC(50)值和文献中报道的那些一致。讨论:本研究证明了一种灵敏且可重现的方法,能够以高通量形式筛选人PARP抑制剂。

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