| Literature DB >> 31858797 |
Jianhua Tian, Kevin B Teuscher, Erin R Aho, Joseph R Alvarado, Jonathan J Mills, Kenneth M Meyers, Rocco D Gogliotti, Changho Han, Jonathan D Macdonald, Jiqing Sai, J Grace Shaw, John L Sensintaffar, Bin Zhao, Tyson A Rietz, Lance R Thomas, William G Payne, William J Moore1, Gordon M Stott1, Jumpei Kondo2,3, Masahiro Inoue2,3, Robert J Coffey, William P Tansey, Shaun R Stauffer, Taekyu Lee, Stephen W Fesik.
Abstract
WD repeat domain 5 (WDR5) is a member of the WD40-repeat protein family that plays a critical role in multiple chromatin-centric processes. Overexpression of WDR5 correlates with a poor clinical outcome in many human cancers, and WDR5 itself has emerged as an attractive target for therapy. Most drug-discovery efforts center on the WIN site of WDR5 that is responsible for the recruitment of WDR5 to chromatin. Here, we describe discovery of a novel WDR5 WIN site antagonists containing a dihydroisoquinolinone bicyclic core using a structure-based design. These compounds exhibit picomolar binding affinity and selective concentration-dependent antiproliferative activities in sensitive MLL-fusion cell lines. Furthermore, these WDR5 WIN site binders inhibit proliferation in MYC-driven cancer cells and reduce MYC recruitment to chromatin at MYC/WDR5 co-bound genes. Thus, these molecules are useful probes to study the implication of WDR5 inhibition in cancers and serve as a potential starting point toward the discovery of anti-WDR5 therapeutics.Entities:
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Year: 2020 PMID: 31858797 PMCID: PMC6986559 DOI: 10.1021/acs.jmedchem.9b01608
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446