Mechanistic study of dual-function inhibitors targeting topoisomerase II and Rad51-mediated DNA repair pathway against castration-resistant prostate cancer.
Yi-Chang ChiangWohn-Jenn LeuYi-Chin ChenPei-Chen YeYu-Tung HsuYu-Chi HsiaoJui-Ling HsuShe-Hung ChanLih-Ching HsuHsu-Shan HuangJih-Hwa GuhPublished in: The Prostate (2023)
The data suggest that WC-A compounds exhibit anti-CRPC effects through the inhibition of TOP II activities, leading to mitochondrial stress-involved caspase activation and apoptosis. Moreover, WC-A13, WC-A14, and WC-A15 but not WC-A16 display inhibitory activities of Rad51-mediated DNA repair pathway which may increase apoptotic effect of CRPC cells.