| Literature DB >> 33596073 |
Peter S Dragovich1, Thomas H Pillow1, Robert A Blake1, Jack D Sadowsky1, Emel Adaligil1, Pragya Adhikari1, Jinhua Chen2, Nicholas Corr1, Josefa Dela Cruz-Chuh1, Geoffrey Del Rosario1, Aaron Fullerton1, Steven J Hartman1, Fan Jiang3, Susan Kaufman1, Tracy Kleinheinz1, Katherine R Kozak1, Liling Liu1, Ying Lu2, Melinda M Mulvihill1, Jeremy M Murray1, Aimee O'Donohue1, Rebecca K Rowntree1, William S Sawyer1, Leanna R Staben1, John Wai2, Jian Wang2, BinQing Wei1, Wentao Wei3, Zijin Xu2, Hui Yao2, Shang-Fan Yu1, Donglu Zhang1, Hongyan Zhang2, Shenhua Zhang3, Yongxin Zhao2, Hao Zhou2, Xiaoyu Zhu2.
Abstract
Heterobifunctional compounds that direct the ubiquitination of intracellular proteins in a targeted manner via co-opted ubiquitin ligases have enormous potential to transform the field of medicinal chemistry. These chimeric molecules, often termed proteolysis-targeting chimeras (PROTACs) in the chemical literature, enable the controlled degradation of specific proteins via their direction to the cellular proteasome. In this report, we describe the second phase of our research focused on exploring antibody-drug conjugates (ADCs), which incorporate BRD4-targeting chimeric degrader entities. We employ a new BRD4-binding fragment in the construction of the chimeric ADC payloads that is significantly more potent than the corresponding entity utilized in our initial studies. The resulting BRD4-degrader antibody conjugates exhibit potent and antigen-dependent BRD4 degradation and antiproliferation activities in cell-based experiments. Multiple ADCs bearing chimeric BRD4-degrader payloads also exhibit strong, antigen-dependent antitumor efficacy in mouse xenograft assessments that employ several different tumor models.Entities:
Year: 2021 PMID: 33596073 DOI: 10.1021/acs.jmedchem.0c01846
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446