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Assay strategies for identification of therapeutic leads that target protein trafficking

机译:鉴定靶向蛋白质运输的治疗线索的测定策略

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摘要

Receptors, enzymes, and ion channels are traditional targets of therapeutic development. A common strategy is to target these proteins with agents that either activate or suppress their activity with ligands or substrates that occupy orthosteric sites or have allosteric interactions. An alternative approach involves regulation of protein trafficking. In principle, this approach enables 'rescue' of misfolded and misrouted mutant proteins to restore function, 'shipwrecking' of undesirable proteins by targeting them for destruction, and regulation of levels of partially expressed wild type (WT) proteins at their functional sites of action. Here, we present drug discovery strategies that identify 'pharmacoperones', which are small molecules that serve as molecular templates and cause otherwise misfolded mutant proteins to fold and route correctly.
机译:受体,酶和离子通道是治疗发展的传统目标。一种常见的策略是用能够激活或抑制其活性的配体或底物占据正构位点或具有变构相互作用的试剂靶向这些蛋白质。一种替代方法涉及调节蛋白质运输。原则上,这种方法能够“挽救”错误折叠和路线错误的突变蛋白以恢复功能,通过将不想要的蛋白作为目标进行破坏来“破坏”,并调节部分表达的野生型(WT)蛋白在其功能位点的水平。在这里,我们提出了识别“ pharmacoperones”的药物发现策略,这些药物是作为分子模板的小分子,会导致错误折叠的突变蛋白正确折叠和传递。

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