秦攀

个人信息Personal Information

副教授

硕士生导师

性别:男

毕业院校:日本国立九州大学

学位:博士

所在单位:控制科学与工程学院

学科:模式识别与智能系统

办公地点:创新园大厦 B713

联系方式:qp112cn@dlut.edu.cn

电子邮箱:qp112cn@dlut.edu.cn

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Inhibition of SGK1 confers vulnerability to redox dysregulation in cervical cancer

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论文类型:期刊论文

发表时间:2019-06-01

发表刊物:REDOX BIOLOGY

收录刊物:SCIE、PubMed

卷号:24

页面范围:101225

ISSN号:2213-2317

关键字:Cervical cancer; SGK1; NRF2; ROS; Melatonin

摘要:Cervical cancer has poor prognosis and patients are often diagnosed at advanced stages of the disease with limited treatment options. There is thus an urgent need for the discovery of new therapeutic strategies in cervical cancer. The activation of SGK1 has been linked to the development of various cancer types but little is known about the role of SGK1 in cervical cancer and its potential as a therapeutic target. Here we report that SGK1 is an antioxidative factor that promotes survival of cervical cancer cells. Gene set enrichment analysis of RNA-Seq data reveals a strong inverse association between SGK1 and oxidative phosphorylation. Consistently, inhibition of SGK1 via siRNA or pharmacological inhibitor GSK650394 induces ROS and cytotoxicity upon H2O2 stress. Further analysis of clinical data associates SGK1 with gene expression signatures regulated by the antioxidant transcription factor NRF2 in cervical cancer. Mechanistically, SGK1 activation exerts antioxidant effect through induction of c-JUN-dependent NRF2 expression and activity. Importantly, we find that inhibition of SGK1 confers vulnerability to melatonin as a pro-oxidant, resulting in ROS over-accumulation and consequently enhanced cell cytotoxicity. We further demonstrate that combined use of GSK650394 and melatonin yields substantial regression of cervical tumors in vivo. This work opens new perspectives on the potential of SGK1 inhibitors as sensitizing agents to enable the design of therapeutically redox-modulating strategies against cervical cancer.