Structure-Based Discovery of CF53 as a Potent and Orally Bioavailable Bromodomain and Extra-Terminal (BET) Bromodomain Inhibitor.
Yujun ZhaoBing ZhouLongchuan BaiLiu LiuChao-Yie YangJennifer L MeagherJeanne A StuckeyDonna McEachernSally PrzybranowskiMi WangXu RanAngelo AguilarYang HuJeff W KampfXiaoqin LiTing ZhaoSiwei LiBo WenDuxin SunShaomeng WangPublished in: Journal of medicinal chemistry (2018)
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 NH-pyrazole group into the 9H-pyrimido[4,5- b]indole core, we identified a series of compounds that bind to BRD4 BD1 protein with Ki 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 in 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.
Keyphrases
- cystic fibrosis
- small molecule
- structural basis
- breast cancer cells
- protein protein
- high throughput
- binding protein
- squamous cell carcinoma
- stem cells
- acute myeloid leukemia
- amino acid
- type diabetes
- machine learning
- bone marrow
- adipose tissue
- molecular docking
- electronic health record
- room temperature
- insulin resistance
- rectal cancer
- mesenchymal stem cells
- ionic liquid
- data analysis