| Literature DB >> 31702389 |
Li-Wen Xia1,2, Meng-Yu Ba1,2, Wei Liu3, Weyland Cheng3, Chao-Ping Hu1,2, Qing Zhao1,2, Yong-Fang Yao1,2, Mo-Ran Sun1,2, Yong-Tao Duan3.
Abstract
Current traditional drugs such as enzyme inhibitors and receptor agonists/antagonists present inherent limitations due to occupancy-driven pharmacology as the mode of action. Proteolysis targeting chimeras (PROTACs) are composed of an E3 ligand, a connecting linker and a target protein ligand, and are an attractive approach to specifically knockdown-targeted proteins utilizing an event-driven mode of action. The length, hydrophilicity and rigidity of connecting linkers play important role in creating a successful PROTAC. Some PROTACs with a triazole linker have displayed promising anticancer activity. This review provides an overview of PROTACs with a triazole scaffold and discusses its structure-activity relationship. Important milestones in the development of PROTACs are addressed and a critical analysis of this drug discovery strategy is also presented.Entities:
Keywords: PROTACs; SAR; drug development; protein degradation; triazole
Year: 2019 PMID: 31702389 DOI: 10.4155/fmc-2019-0159
Source DB: PubMed Journal: Future Med Chem ISSN: 1756-8919 Impact factor: 3.808