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通过基于时间分辨荧光共振能量转移的高通量筛选测定法发现Rho激酶2抑制剂的新型支架

Discovery of novel scaffolds for Rho kinase 2 inhibitor through TRFRET-based high throughput screening assay.

作者信息

Oh Kwang-Seok, Mun Jihye, Cho Jae Eun, Lee Sunghou, Yi Kyu Yang, Lim Chae Jo, Lee Jin Soo, Park Whui Jung, Lee Byung Ho

机构信息

Bio-Organic Science Division, Korea Research Institute of Chemical Technology, Yuseong, Daejeon, Republic of Korea.

出版信息

Comb Chem High Throughput Screen. 2013 Jan;16(1):37-46. doi: 10.2174/1386207311316010006.

Abstract

Recent advances in basic and clinical studies have identified Rho kinase (ROCK) as an important target potentially implicated in a variety of cardiovascular diseases and ROCK inhibitors were considered as a pharmacological strategy to prevent and treat cardiovascular diseases. To screen the small molecule compound library against ROCK, a high throughput screening (HTS) campaign was carried out using immobilized metal affinity for phosphochemicals (IMAP)-based time-resolved fluorescence resonance energy transfer (TR-FRET) assay. Z' value and signal to background (S/B) ratio were achieved at 0.76 and 5.27 for the pilot library screening of the most diverse set consisting of 15,040 compounds with a reasonable reconfirmation rate. From this screening campaign, four novel scaffolds, such as 3- nitropyridine, 4-methoxy-1,3,5,-triazine, naphthalene-1,4-dione, and 2,3-dihydro-1H-pyrrolo[2,3-b]quinoxaline, were yielded. Particularly, we found that 3-nitropyridine derivatives possess potent inhibitory activity and selectivity for ROCK. Our findings provide important information for the design of novel ROCK inhibitor.

摘要

基础和临床研究的最新进展已确定Rho激酶(ROCK)是一个可能与多种心血管疾病相关的重要靶点,并且ROCK抑制剂被视为预防和治疗心血管疾病的一种药理学策略。为了筛选针对ROCK的小分子化合物库,使用基于固定化金属亲和磷化学(IMAP)的时间分辨荧光共振能量转移(TR-FRET)测定法进行了高通量筛选(HTS)。对于由15,040种化合物组成的最多样化集合的先导库筛选,Z'值和信噪比(S/B)分别达到0.76和5.27,且重新确认率合理。通过这次筛选,得到了四种新型骨架,如3-硝基吡啶、4-甲氧基-1,3,5-三嗪、萘-1,4-二酮和2,3-二氢-1H-吡咯并[2,3-b]喹喔啉。特别地,我们发现3-硝基吡啶衍生物对ROCK具有强大的抑制活性和选择性。我们的研究结果为新型ROCK抑制剂的设计提供了重要信息。

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