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用于鉴定ROCK-II抑制剂的滤膜结合法和荧光偏振检测法之间比较的数据一致性。

Data concordance from a comparison between filter binding and fluorescence polarization assay formats for identification of ROCK-II inhibitors.

作者信息

Hubert Cassandra L, Sherling Stacy E, Johnston Patricia A, Stancato Louis F

机构信息

Eli Lilly and Company, Research Triangle Park, NC 27709, USA.

出版信息

J Biomol Screen. 2003 Aug;8(4):399-409. doi: 10.1177/1087057103255071.

Abstract

The Rho-associated coiled-coil-containing protein serine/threonine kinases ROCK-I and ROCK-II are thought to play a major role in cytoskeletal dynamics by serving as downstream effectors of the Rho/Rac family of cytokine- and growth factor-activated small GTPases. As such, the ROCK family members are attractive intervention targets for a variety of pathologies, including cancer and cardiovascular disease. The authors developed a high-throughput screen to identify ROCK-II inhibitors and report results from a direct comparison of 2 screening campaigns for ROCK-II inhibitors using fluorescence polarization (FP) and filter binding (FB). Screening protocols to identify inhibitors of ROCK-II were developed in FB and FP formats under similar assay and kinetic conditions. A 30,000-member compound library was screened using FB ((33)P) and FP detection systems, and compounds that were active in either assay were retested in 5-point curve confirmation assays. Analysis of these data showed an approximate 95% agreement of compounds identified as active in both assay formats. Also, compound potency determinations from FB and FP had a high degree of correlation and were considered equivalent. These data suggest that the assay methodology has little impact on the quality and productivity of the screen, provided that the assays are developed to standardize kinetic conditions.

摘要

含Rho相关卷曲螺旋结构的蛋白丝氨酸/苏氨酸激酶ROCK-I和ROCK-II,被认为通过充当细胞因子和生长因子激活的小GTP酶的Rho/Rac家族的下游效应器,在细胞骨架动力学中发挥主要作用。因此,ROCK家族成员是包括癌症和心血管疾病在内的多种疾病有吸引力的干预靶点。作者开发了一种高通量筛选方法来鉴定ROCK-II抑制剂,并报告了使用荧光偏振(FP)和滤膜结合(FB)对ROCK-II抑制剂进行的2次筛选活动的直接比较结果。在相似的测定和动力学条件下,以FB和FP形式开发了鉴定ROCK-II抑制剂的筛选方案。使用FB((33)P)和FP检测系统对一个包含30000个成员的化合物库进行筛选,在两种测定中具有活性的化合物在5点曲线确认试验中重新进行测试。对这些数据的分析表明,在两种测定形式中被鉴定为具有活性的化合物的一致性约为95%。此外,由FB和FP测定的化合物效力具有高度相关性,并被认为是等效的。这些数据表明,只要开发的测定方法能够标准化动力学条件,测定方法对筛选的质量和效率影响很小。

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