| Literature DB >> 32302140 |
Paul R Leger1, Dennis X Hu1, Berenger Biannic1, Minna Bui1, Xinping Han1, Emily Karbarz1, Jack Maung1, Akinori Okano1, Maksim Osipov1, Grant M Shibuya1, Kyle Young1, Christopher Higgs2, Betty Abraham1, Delia Bradford1, Cynthia Cho1, Christophe Colas1, Scott Jacobson1, Yamini M Ohol1, Deepa Pookot1, Payal Rana1, Jerick Sanchez1, Niket Shah1, Michael Sun1, Steve Wong1, Dirk G Brockstedt1, Paul D Kassner1, Jacob B Schwarz1, David J Wustrow1.
Abstract
USP7 is a promising target for cancer therapy as its inhibition is expected to decrease function of oncogenes, increase tumor suppressor function, and enhance immune function. Using a structure-based drug design strategy, a new class of reversible USP7 inhibitors has been identified that is highly potent in biochemical and cellular assays and extremely selective for USP7 over other deubiquitinases. The succinimide was identified as a key potency-driving motif, forming two strong hydrogen bonds to the allosteric pocket of USP7. Redesign of an initial benzofuran-amide scaffold yielded a simplified ether series of inhibitors, utilizing acyclic conformational control to achieve proper amine placement. Further improvements were realized upon replacing the ether-linked amines with carbon-linked morpholines, a modification motivated by free energy perturbation (FEP+) calculations. This led to the discovery of compound 41, a highly potent, selective, and orally bioavailable USP7 inhibitor. In xenograft studies, compound 41 demonstrated tumor growth inhibition in both p53 wildtype and p53 mutant cancer cell lines, demonstrating that USP7 inhibitors can suppress tumor growth through multiple different pathways.Entities:
Year: 2020 PMID: 32302140 DOI: 10.1021/acs.jmedchem.0c00245
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446