Korona Boguslawa, Itzhaki Laura S
Department of Pharmacology, University of Cambridge, Cambridge, United Kingdom.
J Biol Chem. 2024 Dec;300(12):107926. doi: 10.1016/j.jbc.2024.107926. Epub 2024 Oct 23.
We are now in the middle of a so-called "fourth wave" of drug innovation: multispecific medicines aimed at diseases and targets previously thought to be "undruggable"; by inducing proximity between two or more proteins, for example, a target and an effector that do not naturally interact, such modalities have potential far beyond the scope of conventional drugs. In particular, targeted protein degradation (TPD) strategies to destroy disease-associated proteins have emerged as an exciting pipeline in drug discovery. Most efforts are focused on intracellular proteins, whereas membrane proteins have been less thoroughly explored despite the fact that they comprise roughly a quarter of the human proteome with G-protein coupled receptors (GPCRs) notably dysregulated in many diseases. Here, we discuss the opportunities and challenges of developing degraders for membrane proteins with a focus on GPCRs. We provide an overview of different TPD platforms in the context of membrane-tethered targets, and we present recent degradation technologies highlighting their potential application to GPCRs.
我们目前正处于所谓药物创新的“第四波”之中:针对先前被认为“不可成药”的疾病和靶点的多特异性药物;例如,通过诱导两种或更多种原本不会自然相互作用的蛋白质(如一个靶点和一个效应器)之间的接近,此类药物形式具有远超传统药物范畴的潜力。特别是,用于破坏与疾病相关蛋白质的靶向蛋白质降解(TPD)策略已成为药物研发中一条令人兴奋的途径。大多数研究工作都集中在细胞内蛋白质上,而膜蛋白尽管约占人类蛋白质组的四分之一,且G蛋白偶联受体(GPCRs)在许多疾病中明显失调,但对其研究却不够深入。在此,我们将重点讨论针对GPCRs开发膜蛋白降解剂的机遇与挑战。我们将在膜结合靶点的背景下概述不同的TPD平台,并介绍近期的降解技术,突出其在GPCRs方面的潜在应用。
