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Versatile assays for high throughput screening for activators or inhibitors of intracellular proteases and their cellular regulators.

机译:用于高通量筛选细胞内蛋白酶活化剂或抑制剂及其细胞调节剂的通用检测方法。

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摘要

BACKGROUND: Intracellular proteases constitute a class of promising drug discovery targets. Methods for high throughput screening against these targets are generally limited to in vitro biochemical assays that can suffer many technical limitations, as well as failing to capture the biological context of proteases within the cellular pathways that lead to their activation. METHODS #ENTITYSTARTX00026; FINDINGS: We describe here a versatile system for reconstituting protease activation networks in yeast and assaying the activity of these pathways using a cleavable transcription factor substrate in conjunction with reporter gene read-outs. The utility of these versatile assay components and their application for screening strategies was validated for all ten human Caspases, a family of intracellular proteases involved in cell death and inflammation, including implementation of assays for high throughput screening (HTS) of chemical libraries and functional screening of cDNA libraries. The versatility of the technology was also demonstrated for human autophagins, cysteine proteases involved in autophagy. CONCLUSIONS: Altogether, the yeast-based systems described here for monitoring activity of ectopically expressed mammalian proteases provide a fascile platform for functional genomics and chemical library screening.
机译:背景:细胞内蛋白酶构成了一类有前途的药物发现靶标。针对这些靶标进行高通量筛选的方法通常限于体外生化分析,该方法可能会遭受许多技术限制,并且无法捕获导致其活化的细胞途径中蛋白酶的生物学背景。方法#ENTITYSTARTX00026;结果:我们在这里描述了一个多功能的系统,用于重构酵母中的蛋白酶激活网络,并使用可裂解的转录因子底物和报告基因的读数来分析这些途径的活性。这些通用的测定成分的实用性及其在筛选策略中的应用已针对所有十种人类Caspases(一种参与细胞死亡和炎症的胞内蛋白酶家族)进行了验证,包括实施用于化学文库的高通量筛选(HTS)和功能筛选的测定cDNA文库。还证明了该技术对于人自噬,参与自噬的半胱氨酸蛋白酶的多功能性。结论:总的来说,这里描述的基于酵母的系统用于监测异位表达的哺乳动物蛋白酶的活性,为功能基因组学和化学文库筛选提供了方便的平台。

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