par Brahma, Manoja Kumar 
;Gilglioni, Eduardo Hideo ;Zhou, Lang;Trepo, Eric ;Chen, Pengyu;Gurzov, Esteban Nicolas
Référence Oncogene
Publication Publié, 2021-11-01
;Gilglioni, Eduardo Hideo ;Zhou, Lang;Trepo, Eric ;Chen, Pengyu;Gurzov, Esteban Nicolas Référence Oncogene
Publication Publié, 2021-11-01
Article révisé par les pairs
| Résumé : | Obesity affects more than 650 million individuals worldwide and is a well-established risk factor for the development of hepatocellular carcinoma (HCC). Oxidative stress can be considered as a bona fide tumor promoter, contributing to the initiation and progression of liver cancer. Indeed, one of the key events involved in HCC progression is excessive levels of reactive oxygen species (ROS) resulting from the fatty acid influx and chronic inflammation. This review provides insights into the different intracellular sources of obesity-induced ROS and molecular mechanisms responsible for hepatic tumorigenesis. In addition, we highlight recent findings pointing to the role of the dysregulated activity of BCL-2 proteins and protein tyrosine phosphatases (PTPs) in the generation of hepatic oxidative stress and ROS-mediated dysfunctional signaling, respectively. Finally, we discuss the potential and challenges of novel nanotechnology strategies to prevent ROS formation in obesity-associated HCC. |
