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首页> 外文期刊>Chembiochem: A European journal of chemical biology >Small-molecule screening and profiling by using automated microscopy
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Small-molecule screening and profiling by using automated microscopy

机译:使用自动显微镜对小分子进行筛选和分析

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Automated fluorescence microscopy provides a powerful tool for analyzing the physiological state of single cells with high throughput and high information content. Here I discuss two types of experiments in which this technology was used to discover and characterize bioactive small molecules. In phenotypic-screening experiments, the goal is to find "hits" with specific effects on cells by screening large libraries of small molecules. An example is screening for small molecules that perturb mitosis by novel mechanisms. In cytological-profiling experiments, the goal is to characterize the bioactivity of a limited number of small molecules in considerable depth, and thus understand their mechanism and toxicities at the cellular level. I discuss an example in which 700 small molecules with known bioactivity were profiled by using multiple fluorescent probes, and clustered into mechanistic classes by automated statistical analysis.
机译:自动化荧光显微镜为分析具有高通量和高信息含量的单细胞的生理状态提供了强大的工具。在这里,我讨论了使用该技术发现和表征生物活性小分子的两种类型的实验。在表型筛选实验中,目标是通过筛选大型小分子文库,找到对细胞具有特定作用的“命中”。一个例子是通过新机制筛选干扰有丝分裂的小分子。在细胞学分析实验中,目标是表征相当数量深度的有限数量的小分子的生物活性,从而了解它们在细胞水平上的机制和毒性。我讨论了一个示例,其中使用多个荧光探针对700个具有已知生物活性的小分子进行了分析,并通过自动统计分析将其分为机械类。

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