| Literature DB >> 30661989 |
Qing Ye1, Yinan Zhang2, Yanan Cao1, Xiachang Wang2, Yubin Guo1, Jing Chen3, Jamie Horn4, Larissa V Ponomareva4, Luksana Chaiswing5, Khaled A Shaaban4, Qiou Wei5, Bradley D Anderson6, Daret K St Clair5, Haining Zhu3, Markos Leggas6, Jon S Thorson7, Qing-Bai She8.
Abstract
Peroxiredoxin 1 (Prx1) and glutaredoxin 3 (Grx3) are two major antioxidant proteins that play a critical role in maintaining redox homeostasis for tumor progression. Here, we identify the prototypical pyranonaphthoquinone natural product frenolicin B (FB) as a selective inhibitor of Prx1 and Grx3 through covalent modification of active-site cysteines. FB-targeted inhibition of Prx1 and Grx3 results in a decrease in cellular glutathione levels, an increase of reactive oxygen species (ROS), and concomitant inhibition of cancer cell growth, largely by activating the peroxisome-bound tuberous sclerosis complex to inhibit mTORC1/4E-BP1 signaling axis. FB structure-activity relationship studies reveal a positive correlation between inhibition of 4E-BP1 phosphorylation, ROS-mediated cancer cell cytotoxicity, and suppression of tumor growth in vivo. These findings establish FB as the most potent Prx1/Grx3 inhibitor reported to date and also notably highlight 4E-BP1 phosphorylation status as a potential predictive marker in response to ROS-based therapies in cancer. Published by Elsevier Ltd.Entities:
Keywords: 4E-BP1; AKT; RAS; ROS; eIF4E; frenolicin B; glutaredoxin 3; mTORC1; peroxiredoxin 1; pyranonaphthoquinone
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Year: 2019 PMID: 30661989 PMCID: PMC6557261 DOI: 10.1016/j.chembiol.2018.11.013
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116