UHRF1 promotes renal cell carcinoma progression through epigenetic regulation of TXNIP

被引:0
|
作者
Dian Jiao
Yi Huan
Jia Zheng
Ming Wei
Guoxu Zheng
Donghui Han
Jieheng Wu
Wenjin Xi
Feilong Wei
An-Gang Yang
Weijun Qin
He Wang
Weihong Wen
机构
[1] Tangdu Hospital,Department of Urology
[2] Fourth Military Medical University,Department of Radiology
[3] Xijing Hospital,Department of Oncology
[4] Fourth Military Medical University,Department of Urology
[5] The First Affiliated Hospital of Zhengzhou University,Department of Physiology and Pathophysiology
[6] 150th Central Hospital of PLA,Department of Urology
[7] Fourth Military Medical University,State Key Laboratory of Cancer Biology, Department of Immunology
[8] Xijing Hospital,Department of Orthopedics
[9] Fourth Military Medical University,undefined
[10] Fourth Military Medical University,undefined
[11] Tangdu Hospital,undefined
[12] Fourth Military Medical University,undefined
来源
Oncogene | 2019年 / 38卷
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学科分类号
摘要
UHRF1 is an important epigenetic regulator that belongs to the UHRF family. Overexpression of UHRF1 has been found in many kinds of tumors and its overexpression is associated with poor prognosis and short survival in certain cancer types. However, its function in renal cell carcinoma (RCC) is not clear. Here we report that RCC tumor tissues had obviously higher UHRF1 expression than normal renal tissues. Downregulation of UHRF1 by siRNA or shRNA in RCC cell lines resulted in decreased cell viability, inhibited cell migration and invasion, and increased apoptosis. UHRF1 knockdown RCC xenografts also resulted in obviously inhibited tumor growth in vivo. After downregulation of UHRF1 in RCC cells, the expression of TXNIP was upregulated. In addition, after UHRF1 and TXNIP were simultaneously downregulated, cell viability and cell invasion increased, whereas cell apoptosis decreased compared with UHRF1 single downregulated cells. We also showed that UHRF1 could recruit HDAC1 to the TXNIP promoter and mediate the deacetylation of histone H3K9, resulting in the inhibition of TXNIP expression. Our results confirm that UHRF1 has oncogenic function in RCC and UHRF1 may promote tumor progression through epigenetic regulation of TXNIP. UHRF1 might be used as a therapeutic target for RCC treatment.
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页码:5686 / 5699
页数:13
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