化学
泛素
机制(生物学)
蛋白质降解
前药
计算生物学
降级(电信)
泛素蛋白连接酶类
细胞生物学
泛素连接酶
药物发现
药物开发
化学生物学
生物化学
小分子
结构-活动关系
药理学
靶蛋白
毒性
血浆蛋白结合
作者
Wei Peng,Xiaoyan Pan,Shiqun Wang,G. Huang,Yu Qian
标识
DOI:10.1021/acs.jmedchem.5c03330
摘要
Proteolysis-targeting chimeras (PROTACs) have emerged as a transformative paradigm in pharmaceutical research. Despite significant progress in PROTACs, they are overwhelmingly dominated by the recruitment of a very restricted subset of canonical E3 ligases (e.g., CRBN and VHL), which hinders their potential therapeutic applications. As a result, recent developments have led to the emergence of PROTACs that utilize nonclassical E3 ligases. Another challenge is systemic toxicity caused by degradation on-target degradation in nonintended tissues, prompting the development of pre-PROTACs to achieve conditional and spatiotemporal modulation of target protein levels. Herein, we provide a comprehensive summary and discussion of recent advancements in PROTACs based on "novel" E3 ligases, as well as PROTAC prodrugs activated by external stimuli and the tumor microenvironment, highlighting prospects for the design of effective and selective PROTACs.
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