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首页> 外文期刊>Chembiochem: A European journal of chemical biology >High-content screening and profiling of drug activity in an automated centrosome-duplication assay
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High-content screening and profiling of drug activity in an automated centrosome-duplication assay

机译:自动化中心体重复测定中的药物活性高内涵筛选和分析

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摘要

Maintenance of centrosome number is essential for cell-cycle progression and genomic stability, but investigation of this regulation has been limited by assay difficulty. We present a fully automated image-based centrosome-duplication assay that is accurate and robust enough for both careful cell-biology studies and high-throughput screening, and employ this assay in a series of chemical-genetic studies. We observe that a simple cytometric profiling strategy, which is based on organelle size, groups compounds with similar mechanisms of action; this suggests a simple strategy for excluding compounds that undesirably target such activities as protein synthesis and microtubule dynamics. Screening a library of compounds of known activity, we found unexpected effects on centrosome duplication by a number of drugs, most notably isoform-specific protein kinase C inhibitors and retinoic acid receptor agonists. From a 16320-member library of uncharacterized small molecules, we identified five potent centrosome-duplication inhibitors that do not target microtubule dynamics or protein synthesis. The analysis methodology reported here is directly relevant to studies of centrosome regulation in a variety of systems and is adaptable to a wide range of other biological problems.
机译:维持中心体数目对于细胞周期进程和基因组稳定性是必不可少的,但是该调控的研究受到测定难度的限制。我们提出了一种全自动的基于图像的中心体复制测定法,该方法对于仔细的细胞生物学研究和高通量筛选都足够准确和可靠,并在一系列化学遗传研究中采用了该测定法。我们观察到,基于细胞器大小的简单细胞计数分析策略将具有相似作用机理的化合物分组。这暗示了一种简单的策略,可以排除不希望的靶向诸如蛋白质合成和微管动力学等活性的化合物。筛选具有已知活性的化合物的文库,我们发现许多药物对中心体复制有意想不到的影响,其中最著名的是异构体特异性蛋白激酶C抑制剂和视黄酸受体激动剂。从一个16320个成员的未表征小分子库中,我们鉴定了五种有效的中心体复制抑制剂,它们不针对微管动力学或蛋白质合成。此处报告的分析方法与各种系统中中心体调节的研究直接相关,并且适用于多种其他生物学问题。

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