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Parallel Chemical Genetic and Genome-Wide RNAi Screens Identify Cytokinesis Inhibitors and Targets

机译:平行化学遗传和基因组RNAi屏幕识别细胞因子抑制剂和目标

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Cytokinesis involves temporally and spatially coordinated action of the cell cycle and cytoskeletal and membrane systems to achieve separation of daughter cells. To dissect cytokinesis mechanisms it would be useful to have a complete catalog of the proteins involved, and small molecule tools for specifically inhibiting them with tight temporal control. Finding active small molecules by cell-based screening entails the difficult step of identifying their targets. We performed parallel chemical genetic and genome-wide RNA interference screens in Drosophila cells, identifying 50 small molecule inhibitors of cytokinesis and 214 genes important for cytokinesis, including a new protein in the Aurora B pathway (Borr). By comparing small molecule and RNAi phenotypes, we identified a small molecule that inhibits the Aurora B kinase pathway. Our protein list provides a starting point for systematic dissection of cytokinesis, a direction that will be greatly facilitated by also having diverse small molecule inhibitors, which we have identified. Dissection of the Aurora B pathway, where we found a new gene and a specific small molecule inhibitor, should benefit particularly. Our study shows that parallel RNA interference and small molecule screening is a generally useful approach to identifying active small molecules and their target pathways.
机译:细胞因子涉及细胞周期和细胞骨骼和膜系统的时间和空间协调作用,以实现子细胞的分离。解剖细胞因子机制,具有所涉及的蛋白质的完整目录是有用的,以及用于特异性抑制它们的小型时间控制的小分子工具。通过基于细胞的筛选找到活跃的小分子需要识别目标的艰难步骤。我们在果蝇细胞中进行了平行化学遗传和基因组RNA干扰筛,鉴定了50个细胞因子的小分子抑制剂和对细胞因子的214个基因重要,包括Aurora B途径(Borr)中的新蛋白质。通过比较小分子和RNAi表型,我们鉴定了一种抑制极光B激酶途径的小分子。我们的蛋白质清单提供了细胞因子的系统解剖的起点,这是通过我们鉴定的多样性小分子抑制剂来极大地促进的方向。剖析性Aurora B途径,我们发现新的基因和特定的小分子抑制剂,应特别有益。我们的研究表明,并行RNA干扰和小分子筛选是鉴定活性小分子及其靶途径的一种通常有用的方法。

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