| Literature DB >> 28892380 |
F Anthony Romero1, Jeremy Murray1, Kwong Wah Lai2, Vickie Tsui1, Brian K Albrecht3, Le An1, Maureen H Beresini1, Gladys de Leon Boenig1, Sarah M Bronner1, Emily W Chan1, Kevin X Chen2, Zhongguo Chen2, Edna F Choo1, Kyle Clagg1, Kevin Clark1, Terry D Crawford1, Patrick Cyr1, Denise de Almeida Nagata1, Karen E Gascoigne1, Jane L Grogan1, Georgia Hatzivassiliou1, Wei Huang2, Thomas L Hunsaker1, Susan Kaufman1, Stefan G Koenig1, Ruina Li1, Yingjie Li2, Xiaorong Liang1, Jiangpeng Liao2, Wenfeng Liu2, Justin Ly1, Jonathan Maher1, Colin Masui1, Mark Merchant1, Yingqing Ran1, Alexander M Taylor3, John Wai2, Fei Wang2, Xiaocang Wei2, Dong Yu2, Bing-Yan Zhu1, Xiaoyu Zhu2, Steven Magnuson1.
Abstract
Inhibition of the bromodomain of the transcriptional regulator CBP/P300 is an especially interesting new therapeutic approach in oncology. We recently disclosed in vivo chemical tool 1 (GNE-272) for the bromodomain of CBP that was moderately potent and selective over BRD4(1). In pursuit of a more potent and selective CBP inhibitor, we used structure-based design. Constraining the aniline of 1 into a tetrahydroquinoline motif maintained potency and increased selectivity 2-fold. Structure-activity relationship studies coupled with further structure-based design targeting the LPF shelf, BC loop, and KAc regions allowed us to significantly increase potency and selectivity, resulting in the identification of non-CNS penetrant 19 (GNE-781, TR-FRET IC50 = 0.94 nM, BRET IC50 = 6.2 nM; BRD4(1) IC50 = 5100 nΜ) that maintained good in vivo PK properties in multiple species. Compound 19 displays antitumor activity in an AML tumor model and was also shown to decrease Foxp3 transcript levels in a dose dependent manner.Entities:
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Year: 2017 PMID: 28892380 DOI: 10.1021/acs.jmedchem.7b00796
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446