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首页> 外文期刊>Expert opinion on therapeutic targets >Defining interacting partners for drug discovery.
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Defining interacting partners for drug discovery.

机译:定义相互作用的伙伴以进行药物发现。

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摘要

Over the past few years, several technologies have been developed to determine interacting partners of proteins. The techniques fall into two broad categories: direct and indirect. Experimental techniques have been developed to directly probe protein interactions by monitoring protein-binding events. These techniques include the two-hybrid approach, protein fragment complementation assays, co-purification techniques and protein chips. In addition to these methodologies, several approaches have also emerged over the past few years to deduce indirect couplings between proteins. These couplings do not necessarily imply that two proteins are bound within the cell; however, they do provide evidence that perturbing one protein is likely to significantly perturb the function of its partner. These couplings may be deduced by studying the evolution of protein pairs, estimating the degree of correlated transcription of two genes, searching for synthetic lethal pairs, or identifying the chromosomal binding sites of transcriptional regulators. In all cases, protein interactions and protein couplings are being used to advance drug discovery by providing detailed information on protein functions, and by suggesting novel targets that act within biochemical pathways implicated in disease.
机译:在过去的几年中,已经开发了几种技术来确定蛋白质的相互作用伴侣。这些技术分为两大类:直接技术和间接技术。已经开发了通过监测蛋白质结合事件来直接探测蛋白质相互作用的实验技术。这些技术包括“双杂交”方法,蛋白质片段互补分析,共纯化技术和蛋白质芯片。除了这些方法,在过去几年中还出现了几种推断蛋白质之间间接偶联的方法。这些偶联并不一定意味着两种蛋白质会在细胞内结合;而是在细胞内结合。但是,它们确实提供了证据,证明干扰一种蛋白质可能会大大干扰其伴侣的功能。这些偶联可以通过研究蛋白质对的进化,估计两个基因的相关转录程度,寻找合成的致死对或鉴定转录调节子的染色体结合位点来推导。在所有情况下,都通过提供蛋白质功能的详细信息,并建议在涉及疾病的生化途径中起作用的新靶标,利用蛋白质相互作用和蛋白质偶联来促进药物开发。

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