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Recent advances and method development for drug target identification.

机译:用于药物靶标鉴定的最新进展和方法开发。

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摘要

Although it is commonly recognized that most drugs cause inhibition or activation of function by physically binding to one or more gene products, the direct interactions of bioactive small molecules with specific gene products, or targets, is often not well characterized. From a therapeutic perspective, it is nevertheless essential to know a drug's binding partner(s) to understand the mechanism of action and anticipate possible side effects to avoid costly clinical failures. This knowledge is increasingly important as the prevalence of polypharmacy expands to include drugs that engage multiple targets. This review provides a succinct overview of several recent approaches that employ genetics, proteomics, expression profiling or bioinformatics procedures for the systematic characterization of the targets of bioactive compounds. The continuous improvement and advancement of existing technologies is critically discussed and we offer a perspective on the future of innovative emerging new generation technologies.
机译:尽管通常认为大多数药物通过物理结合一种或多种基因产物引起抑制或激活功能,但是生物活性小分子与特定基因产物或靶标的直接相互作用往往没有得到很好的表征。从治疗的角度来看,了解药物的结合伴侣以了解作用机理并预测可能的副作用以避免昂贵的临床失败至关重要。随着多元药房的普及,包括参与多个目标的药物,这种知识变得越来越重要。这篇综述简要概述了使用遗传学,蛋白质组学,表达谱或生物信息学方法对生物活性化合物靶标进行系统表征的几种最新方法。对现有技术的不断改进和进步进行了严格的讨论,我们为创新的新一代技术的未来提供了一个视角。

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