Metabolomics analysis reveals cytotoxic effects of ouabain towards psoriatic keratinocytes via impairment of glutathione metabolism

Author:

Zhou XuanORCID,Fei Fei,Song Wei,Ma Hehua,Xu Zhenzhen,Yue Jing,Cao Bei,Sun Runbin,Zhao Yu,Yang Yuanxun,Jiang Junyi,Geng Yan,Weng Zuyi,Li Juan

Abstract

AbstractOuabain is a cardiac glycoside long studied for treating heart diseases, but the attempts to evaluate its anti-psoriatic activity have not been reported. We aimed to explore the effects of ouabain on proliferation and metabolism towards psoriatic keratinocytes. In human HaCaT keratinocytes, ouabain potently decreased viability, promoted apoptosis and caused G2/M cycle arrest. Metabolomics analysis indicated that ouabain markedly impaired glutathione metabolism. The solute carrier family 7 member 11 (SLC7A11) is an amino acid transporter highly specific to cysteine, which is critical for glutathione synthesis. Ouabain downregulated SLC7A11, reduced cysteine uptake and subsequently inhibited glutathione synthesis, probably through inhibiting Akt/mTOR/beclin axis that regulate protein activity of SLC7A11. The impaired glutathione synthesis and oxidative stress caused by ouabain may contribute to its cytotoxicity towards psoriatic keratinocytes. Our results provide experimental evidence supporting further study of ouabain as a potential anti-psoriatic agent.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Jiangsu Province

the Science and Technology Development Project of Jiangsu Provincial Bureau of Traditional Chinese Medicine

Publisher

Springer Science and Business Media LLC

Subject

Genetics,Molecular Biology,General Medicine

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