Mitochondrial Uncouplers Inhibit Oncogenic E2F1 Activity and Prostate Cancer Growth

Overview

Journal Cell Rep Med

Publisher Cell Press

Date 2025 Jan 10

PMID 39793570

Authors

Ohuod Hawsawi

Weinan Xue

Tingting Du

Mengqi Guo

Xiaolin Yu

Mingyi Zhang

Paul S Hoffman

Roni Bollag

Jun Li

Jia Zhou

Hongbo Wang

Junran Zhang

Zheng Fu

Xiaoguang Chen

Chunhong Yan

Affiliations

Soon will be listed here.

Abstract

Mitochondrial uncouplers dissipate proton gradients and deplete ATP production from oxidative phosphorylation (OXPHOS). While the growth of prostate cancer depends on OXPHOS-generated ATP, the oncogenic pathway mediated by the transcription factor E2F1 is crucial for the progression of this deadly disease. Here, we report that mitochondrial uncouplers, including tizoxanide (TIZ), the active metabolite of the Food and Drug Administration (FDA)-approved anthelmintic nitazoxanide (NTZ), inhibit E2F1-mediated expression of genes involved in cell cycle progression, DNA synthesis, and lipid synthesis. Consequently, NTZ/TIZ induces S-phase kinase-associated protein 2 (SKP2)-mediated G1 arrest while impeding DNA synthesis, lipogenesis, and the growth of prostate cancer cells. The anti-cancer activity of TIZ correlates with its OXPHOS-uncoupling activity. NTZ/TIZ appears to inhibit ATP production, thereby activating the AMP-activated kinase (AMPK)-p38 pathway, leading to cyclin D1 degradation, Rb dephosphorylation, and subsequent E2F1 inhibition. Our results thus connect OXPHOS uncoupling to the inhibition of an essential oncogenic pathway, supporting repositioning NTZ and other mitochondrial uncouplers for prostate cancer therapy.

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