SIRT1‐mediated transcriptional regulation of SOX2 is important for self‐renewal of liver cancer stem cells

Liu, Limei; Liu, Chungang; Zhang, Qianzhen; Shen, Junjie; Zhang, Heng; Shan, Juanjuan; Duan, Guangjie; Guo, Deyu; Chen, Xuejiao; Cheng, Jiamin; Xu, Yan; Yang, Zhi; Yao, Chao; Lai, Maode; Qian, Cheng

doi:10.1002/hep.28690

Cited by 91 publications

(97 citation statements)

References 45 publications

(54 reference statements)

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“…These observations are further corroborated by patient‐based studies that Sox2 is the most increased gene among core pluripotency factors in premalignant cirrhotic liver, where hepatocytes have already become resistant to TGFβ‐induced mitoinhibition/apoptosis . In addition to being considered as a predictor for poor survival of HCC patients, Sox2 has also been shown to play an essential role in self‐renewal and maintenance of cancer stem‐like cell populations in HCC . Therefore, TGF‐β signaling may counterbalance Sox2 in cancer initiating and progenitor cell differentiation.…”

Section: Discussionmentioning

confidence: 62%

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A Transforming Growth Factor‐β and H19 Signaling Axis in Tumor‐Initiating Hepatocytes That Regulates Hepatic Carcinogenesis

et al. 2018

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Section: Discussionmentioning

confidence: 62%

“…(40) In addition to being considered as a predictor for poor survival of HCC patients, (41) Sox2 has also been shown to play an essential role in self-renewal and maintenance of cancer stem-like cell populations in HCC. (42) Therefore, TGF-β signaling may counterbalance Sox2 in cancer initiating and progenitor cell differentiation.…”

Section: Discussionmentioning

confidence: 99%

A Transforming Growth Factor‐β and H19 Signaling Axis in Tumor‐Initiating Hepatocytes That Regulates Hepatic Carcinogenesis

et al. 2018

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“…It plays important roles in cell proliferation, apoptosis, aging, inflammation and metabolism (30–32). In addition, it can affect tumorigenesis, development and metastasis of a tumor (33,34). Sirt1 is heterogeneously expressed in tumor, which is closely related to tumor types.…”

Section: Discussionmentioning

confidence: 99%

miR-138 suppresses the proliferation, metastasis and autophagy of non-small cell lung cancer by targeting Sirt1

Fang

Pan

et al. 2017

Oncology Reports

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The present study determined the role and mechanism of miR-138 in non-small cell lung cancer (NSCLC). In total, 45 freshly resected clinical NSCLC tissues were collected. The expression of miR-138 in tissues and cell lines were determined by real-time quantitative PCR. miR-138 mimics were transfected into A549 and Calu-3 cells in vitro, and then the effects of miR-138 on lung cancer cell proliferation, cell cycle, invasion and metastasis were investigated by CCK-8 assay, Transwell and flow cytometry, respectively. The protein expression of the potential target gene Sirt1 in lung cancer cells were determined by western blot analysis. Dual-Luciferase reporter assay was performed to further confirm whether Sirt1 was the target gene of miR-138. The expression of miR-138 was significantly lower in lung cancer tissues and was negatively correlated to the differentiation degree and lymph node metastasis of lung cancer. In vitro experiment results showed that miR-138 inhibited lung cancer cell proliferation, invasion and migration. It was verified that miR-138 could downregulate Sirt1 protein expression, inhibit epithelial-mesenchymal transition (EMT), decrease the activity of AMPK signaling pathway and elevate mTOR phosphorylation level. Dual-Luciferase reporter assay demonstrated that miR-138 could directly regulate Sirt1. Downregulation of Sirt1 alone can also cause the same molecular and biological function changes. Western blot analysis and confocal microscopy results indicated that overexpression of miR-138 or interference of Sirt1 expression could inhibit lung cancer cell autophagy activity possibly through AMPK-mTOR signaling pathway. miR-138 plays a tumor suppressor function in lung cancer. It may inhibit the proliferation, invasion and migration of lung cancer through downregulation of Sirt1 expression and activation of cell autophagy. The downregulation of miR-138 is closely related to the development of lung cancer.

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“…More interestingly, the suppressive effects of SOX2 on HBV RNA transcription and HBV protein production are also confirmed in the BALB/c mice sera and liver tissues. We suggested that SOX2 may act as a restriction factor to repress HBV replication, not only during the acute infection, but also in the chronic infection and the development of liver diseases [12,20]. Previous studies have reported that HBV mRNA was lower in the HCC tissues relative to the non-tumor liver tissues [21,22].…”

Section: Discussionmentioning

confidence: 99%

“…SOX2 is also involved in the progression of HCC. For instance, SOX2 is a main downstream regulator of the silent information regulator 1 (SIRT1)-mediated self-renewal and tumorigenicity of liver cancer stem cells [12]. Moreover, overexpression of SOX2 and its co-factor Oct4 can be novel predictors of poor prognosis for patients undergoing resection of HCC [10].…”

Section: Introductionmentioning

confidence: 99%

SOX2 Represses Hepatitis B Virus Replication by Binding to the Viral EnhII/Cp and Inhibiting the Promoter Activation

Yang

et al. 2020

Viruses

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Hepatitis B virus (HBV) replication is controlled by four promoters (preS1, preS2, Cp, and Xp) and two enhancers (EnhI and EnhII). EnhII stimulates Cp activity to regulate the transcriptions of precore, core, polymerase, and pregenomic RNAs, and therefore, EnhII/Cp is essential for the regulation of HBV replication. This study revealed a distinct mechanism underlying the suppression of EnhII/Cp activation and HBV replication. On the one hand, the sex determining region Y box2 (SOX2), a transcription factor, is induced by HBV. On the other hand, SOX2, in turn, represses the expression levels of HBV RNAs, HBV core-associated DNA, hepatitis B surface antigen (HBsAg), and hepatitis B e antigen (HBeAg), thereby playing an inhibitory role during HBV replication. Further studies indicated that SOX2 bound to the EnhII/Cp DNA and repressed the promoter activation. With the deletion of the high mobility group (HMG) domain, SOX2 loses the ability to repress EnhII/Cp activation, viral RNA transcription, HBV core-associated DNA replication, HBsAg and HBeAg production, as well as fails to enter the nucleus, demonstrating that the HMG domain is required for the SOX2-mediated repression of HBV replication. Moreover, SOX2 represses HBsAg and HBeAg secretion in BALB/c mice sera, and attenuates HBV 3.5 kb RNA transcription and hepatitis B virus core protein (HBc) production in the liver tissues, demonstrating that SOX2 suppresses HBV replication in mice. Furthermore, the results revealed that the HMG domain was required for SOX2-mediated repression of HBV replication in the mice. Taken together, the above facts indicate that SOX2 acts as a new host restriction factor to repress HBV replication by binding to the viral EnhII/Cp and inhibiting the promoter activation through the HMG domain.

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SIRT1‐mediated transcriptional regulation of SOX2 is important for self‐renewal of liver cancer stem cells

Cited by 91 publications

References 45 publications

A Transforming Growth Factor‐β and H19 Signaling Axis in Tumor‐Initiating Hepatocytes That Regulates Hepatic Carcinogenesis

A Transforming Growth Factor‐β and H19 Signaling Axis in Tumor‐Initiating Hepatocytes That Regulates Hepatic Carcinogenesis

miR-138 suppresses the proliferation, metastasis and autophagy of non-small cell lung cancer by targeting Sirt1

SOX2 Represses Hepatitis B Virus Replication by Binding to the Viral EnhII/Cp and Inhibiting the Promoter Activation

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