posted on 2022-11-09, 17:12authored byWeijiao Chen, Minghui Ji, Hao Cheng, Mingming Zheng, Fei Xia, Wenjian Min, Huanaoyu Yang, Xiao Wang, Liping Wang, Lijuan Cao, Kai Yuan, Peng Yang
Breast cancer is the most common tumor in women, and
selective
cyclin-dependent kinase (CDK) 4/6 inhibitors played an important role
in the treatment of breast cancer. Therefore, discovering selective
CDK4/6 inhibitors with great safety and potent efficacy is beneficial
for the breast cancer treatment. In our work, the lead compound 8 was identified through virtual screening; then, systematic
structural optimization was conducted to afford 42, which
exhibited strong inhibition on CDK4/6 and showed high selectivity
among 205 kinases. 42 possessed excellent safety profiles
(LD50 > 5,000 mg/kg), favorable pharmacokinetic properties
(F % = 43%), and potent efficacy in reducing the
burden of breast cancer in vivo. In conclusion, we offered a highly
selective CDK4/6 inhibitor, which could be used as a great candidate
for further preclinical studies of breast cancer.