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 Guh

Published 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.

Keyphrases

dna repair
dna damage
cell death
cell cycle arrest
induced apoptosis
oxidative stress
dna damage response
endoplasmic reticulum stress
machine learning
signaling pathway
cell proliferation
big data
stress induced
data analysis