Structure-Based Discovery of CF53 as a Potent and Orally Bioavailable Bromodomain and Extra-Terminal (BET) Bromodomain Inhibitor

被引：34

作者：

Zhao, Yujun ^{[1
,2
,3
,4
,9
]}

Zhou, Bing ^{[1
,2
,3
,4
,9
]}

Bai, Longchuan ^{[1
,2
,3
,4
]}

Liu, Liu ^{[1
,2
,3
,4
]}

Yang, Chao-Yie ^{[1
,2
,3
,4
]}

Meagher, Jennifer L. ^{[5
,6
]}

Stuckey, Jeanne A. ^{[5
,6
]}

McEachern, Donna ^{[1
,2
,3
,4
]}

Przybranowski, Sally ^{[1
,2
,3
,4
]}

Wang, Mi ^{[1
,2
,3
,4
]}

Ran, Xu ^{[1
,2
,3
,4
,10
]}

Aguilar, Angelo ^{[1
,2
,3
,4
]}

Hu, Yang ^{[1
,2
,3
,4
]}

Kampf, Jeff W. ^{[7
]}

Li, Xiaoqin ^{[8
]}

Zhao, Ting ^{[8
]}

Li, Siwei ^{[8
]}

Wen, Bo ^{[8
]}

Sun, Duxin ^{[8
]}

Wang, Shaomeng ^{[1
,2
,3
,4
]}

机构：

[1] Univ Michigan, Coll Pharm, Rogal Canc Ctr, Ann Arbor, MI 48109 USA

[2] Univ Michigan, Coll Pharm, Dept Internal Med, Ann Arbor, MI 48109 USA

[3] Univ Michigan, Coll Pharm, Dept Pharmacol, Ann Arbor, MI 48109 USA

[4] Univ Michigan, Coll Pharm, Dept Med Chem, Ann Arbor, MI 48109 USA

[5] Univ Michigan, Coll Pharm, Life Sci Inst, Ann Arbor, MI 48109 USA

[6] Univ Michigan, Coll Pharm, Dept Biol Chem, Ann Arbor, MI 48109 USA

[7] Univ Michigan, Coll Pharm, Dept Chem, Ann Arbor, MI 48109 USA

[8] Univ Michigan, Coll Pharm, Dept Pharmaceut Sci, Ann Arbor, MI 48109 USA

[9] Chinese Acad Sci, Shanghai Inst Materia Med, State Key Lab Drug Res, Shanghai 201203, Peoples R China

[10] Univ Calif San Francisco, Inst Neurodegenerat Dis, San Francisco, CA 94143 USA

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 2018年 / 61卷 / 14期

关键词：

TRANSCRIPTIONAL REGULATORS; FAMILY; IDENTIFICATION; ACETYLATION; CANDIDATE; CHROMATIN; RVX-208; PROTEIN; TESTIS; BRD4;

D O I：

10.1021/acs.jmedchem.8b00483

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

We report the structure-based discovery of CF53 (28) as a highly potent and orally active inhibitor of bromodomain and extra-terminal (BET) proteins. By the incorporation of a NHpyrazole group into the 9H-pyrimido[4,5-b] indole core, we identified a series of compounds that bind to BRD4 BD1 protein with K-i values of <1 nM and achieve low nanomolar potencies in the cell growth inhibition of leukemia and breast cancer cells. The most-promising compound, CF53, possesses excellent oral pharmacokinetic properties and achieves significant antitumor activity in0 both triple-negative breast cancer and acute leukemia xenograft models in mice. Determination of the co-crystal structure of CF53 with the BRD4 BD1 protein provides a structural basis for its high binding affinity to BET proteins. CF53 is very selective over non-BET bromodomain-containing proteins. These data establish CF53 as a potent, selective, and orally active BET inhibitor, which warrants further evaluation for advanced preclinical development.

引用

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页码：6110 / 6120

页数：11

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