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Systematic polypharmacology and drug repurposing via an integrated L1000-based Connectivity Map database mining

机译:通过集成的基于L1000的连接图数据库挖掘系统的系统性多酚和药物修复

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摘要

Drug repurposing aims to find novel indications of clinically used or experimental drugs. Because drug data already exist, drug repurposing may save time and cost, and bypass safety concerns. Polypharmacology, one drug with multiple targets, serves as a basis for drug repurposing. Large-scale databases have been accumulated in recent years, and utilization and integration of these databases would be highly helpful for polypharmacology and drug repurposing. The Connectivity Map (CMap) is a database collecting gene-expression profiles of drug-treated human cancer cells, which has been widely used for investigation of polypharmacology and drug repurposing. In this study, we integrated the next-generation L1000-based CMap and an analytic Web tool, the L1000FWD, for systematic analyses of polypharmacology and drug repurposing. Two different types of anti-cancer drugs were used as proof-of-concept examples, including histone deacetylase (HDAC) inhibitors and topoisomerase inhibitors. We identified KM-00927 and BRD-K75081836 as novel HDAC inhibitors and mitomycin C as a topoisomerase IIB inhibitor. Our study provides a prime example of utilization and integration of the freely available public resources for systematic polypharmacology analysis and drug repurposing.
机译:药物修复旨在查找临床使用或实验药物的新迹象。因为药物数据已经存在,药物重新淘汰可能节省时间和成本,并绕过安全问题。多药地,一种具有多种靶标的药物,用作药物重新施用的基础。近年来累积了大规模数据库,利用和整合这些数据库对于多药地和药物重新施用非常有用。连接图(CMAP)是收集药物处理的人癌细胞的基因表达谱的数据库,其已被广泛用于调查多酚和药物重新施用。在这项研究中,我们整合了基于下一代L1000的CMAP和一个分析网工具,L1000FWD,用于系统分析多药和药物重新扫描。两种不同类型的抗癌药物被用作概念证据,包括组蛋白脱乙酰酶(HDAC)抑制剂和拓扑异构酶抑制剂。我们将KM-00927和BRD-K75081836鉴定为新型HDAC抑制剂和丝霉素C作为拓扑异构酶IIB抑制剂。我们的研究提供了自由可用的公共资源的利用和整合,以获得系统性多酚乐接分析和药物重新淘汰的奖励和整合。

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