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Evolution of Cereblon-Mediated Protein Degradation as a Therapeutic Modality

机译:大型介导的蛋白质降解作为治疗方式的演变

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Many cellular processes and pathways are mediated by the regulation of protein-protein complexes. For example, E3 ubiquitin ligases recruit substrate proteins and transfer a ubiquitin tag to target those proteins for destruction by the proteasome. It has now been shown that this cellular process for protein destruction can be redirected by small molecules in both laboratory and clinical settings. This presents a new paradigm in drug discovery, enabling the rapid removal of target proteins linked to disease. In this Innovations review, we will describe the work done on cereblon as a case study on the different strategies available for targeted protein degradation.
机译:许多细胞过程和途径由蛋白质 - 蛋白质复合物的调节介导。 例如,E3泛素连接酶募集底物蛋白并转移泛素标签以靶向这些蛋白质以通过蛋白酶体破坏。 现在已经表明,这种用于蛋白质破坏的细胞方法可以通过实验室和临床环境中的小分子重定向。 这提出了一种在药物发现中的新范式,使得能够快速去除与疾病相关的靶蛋白。 在这一创新审查中,我们将描述在席伯隆所做的工作,以案例研究有针对性蛋白质降解的不同策略。

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