Suppression of SIRT6 by miR-33a facilitates tumor growth of glioma through apoptosis and oxidative stress resistance

Chang, Mingze; Lin, Qiao; Li, Bin; Wang, Juanhong; Zhang, Gejuan; Shi, Wenzhen; Liu, Zhiqin; Gu, Naibing; Zhang, Di; Wang, Xinlai; Tian, Ye

doi:10.3892/or.2017.5780

Cited by 38 publications

(28 citation statements)

References 30 publications

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“…Besides, the subcutaneous xenograft model using U251 cells is helpful for understanding the potential mechanism of glioma in vivo. [27][28][29] Here we using the xenograft model further confirmed the anti-tumor role of circ-TTBK2 inhibition in glioma via regulating the miR-1283/CHD1 axis in vivo.…”

Section: Discussionsupporting

confidence: 66%

<p>Knockdown of circ-TTBK2 Inhibits Glioma Progression by Regulating miR-1283 and CHD1</p>

Han

Wang

et al. 2020

CMAR

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Background: Dysregulated circular RNAs (circRNAs) are involved in the development of glioma. This paper aims to analyze the role and mechanism of circRNA tau tubulin kinase 2 (circ-TTBK2) in glioma progression. Methods: The glioma samples and normal brain tissues were collected. The levels of circ-TTBK2, microRNA-1283 (miR-1283) and chromodomain helicase DNA-binding protein 1 (CHD1) were examined via quantitative reverse transcription polymerase chain reaction or Western blot. Cell proliferation, migration, invasion and glycolysis were determined via 3-(4, 5-dimethyl-2-thiazolyl)-2, 5-diphenyl-2-H-tetrazolium bromide, transwell assay, Western blot, glucose and lactate assay kits. The target relationship was analyzed via dualluciferase reporter assay. The xenograft model was established using U251 cells. Results: circ-TTBK2 expression was increased in glioma tissues and cells. circ-TTBK2 knockdown suppressed glioma cell proliferation, migration, invasion and glycolysis. circ-TTBK2 was a sponge for miR-1283, and knockdown of miR-1283 reversed the effect of circ-TTBK2 silence on glioma progression. CHD1 was targeted via miR-1283, and miR-1283 repressed glioma cell proliferation, migration, invasion and glycolysis via decreasing CHD1. Knockdown of circ-TTBK2-reduced CHD1 expression by mediating miR-1283. Silence of circ-TTBK2 reduced xenograft tumor growth. Conclusion: Down-regulation of circ-TTBK2 suppressed glioma development by regulating miR-1283 and CHD1, providing a new mechanism for understanding glioma pathogenesis.

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Section: Discussionsupporting

confidence: 66%

<p>Knockdown of circ-TTBK2 Inhibits Glioma Progression by Regulating miR-1283 and CHD1</p>

Han

Wang

et al. 2020

CMAR

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“…The increased ATP level upon SIRT6 activation states for increased NADH oxidation and nicely correlates with increased ROS production. Moreover, it is reported that overexpression of SIRT6 results in increased ROS production and that a specific miR-33a by suppressing SIRT6 induced tumor growth through oxidative stress resistance 46 . Work is in progress in our laboratory in order to fill this gap.…”

Section: Discussionmentioning

confidence: 99%

Pharmacological activation of SIRT6 triggers lethal autophagy in human cancer cells

Iachettini¹,

Trisciuoglio

Rotili

et al. 2018

Cell Death Dis

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Sirtuin 6 (SIRT6) is a member of the NAD+-dependent class III deacetylase sirtuin family, which plays a key role in cancer by controlling transcription, genome stability, telomere integrity, DNA repair, and autophagy. Here we analyzed the molecular and biological effects of UBCS039, the first synthetic SIRT6 activator. Our data demonstrated that UBCS039 induced a time-dependent activation of autophagy in several human tumor cell lines, as evaluated by increased content of the lipidated form of LC3B by western blot and of autophagosomal puncta by microscopy analysis of GFP-LC3. UBCS039-mediated activation of autophagy was strictly dependent on SIRT6 deacetylating activity since the catalytic mutant H133Y failed to activate autophagy. At the molecular level, SIRT6-mediated autophagy was triggered by an increase of ROS levels, which, in turn, resulted in the activation of the AMPK-ULK1-mTOR signaling pathway. Interestingly, antioxidants were able to completely counteract UBCS039-induced autophagy, suggesting that ROS burst had a key role in upstream events leading to autophagy commitment. Finally, sustained activation of SIRT6 resulted in autophagy-related cell death, a process that was markedly attenuated using either a pan caspases inhibitor (zVAD-fmk) or an autophagy inhibitor (CQ). Overall, our results identified UBCS039 as an efficient SIRT6 activator, thereby providing a proof of principle that modulation of the enzyme can influence therapeutic strategy by enhancing autophagy-dependent cell death.

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“…Downregulation of SIRT6 increases the phosphorylation level of Janus kinase 2 (JAK2) and STAT3, enhancing the JAK2/STAT3 pathway, which attenuates H 2 O 2 -induced oxidative stress and suppresses apoptosis in glioma cells, and thus miR-33a overexpression inhibits apoptosis in glioma (Fig. 6A) (95). Wang et al (96) have demonstrated that miR-33a overexpression downregulates phosphodiesterase 8A (PDE8A) and UV radiation resistance associated (UVRAG), and upregulates their downstream proteins p-CREB and Notch intracellular domain, respectively, in glioma cells.…”

Section: Urinary System Cancermentioning

confidence: 99%

“…Studies have indicated that miR-33a acts as an oncogene in glioma. Chang et al ( 95 ) have revealed that miR-33a is upregulated in glioma cells. Consequently, the miR-33a target sirtuin 6 (SIRT6) is downregulated, reducing the levels of cleaved caspase 8 and BAX, and promoting Bcl-2 expression ( 95 ).…”

Section: Mir-33a and Its Role In Cancermentioning

confidence: 99%

Role of microRNA‑33a in malignant cells (Review)

et al. 2020

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Cancer causes most of the mortality and morbidity worldwide, with a significant increase in incidence during recent years. MicroRNAs (miRNAs/miRs) are non-coding small RNAs capable of regulating gene expression. They regulate crucial cellular processes, including proliferation, differentiation, metastasis and apoptosis. Therefore, abnormal miRNA expression is associated with multiple diseases, including cancer. There are two types of cancer-associated miRNAs, oncogenic and tumor suppressor miRNAs, depending on their roles and expression patterns in cancer. Accordingly, miRNAs are considered to be targets for cancer prevention and treatment. miR-33a controls cellular cholesterol uptake and synthesis, which are both closely associated with carcinogenesis. The present review thoroughly describes the roles of miR-33a in more than a dozen types of cancer and the underlying mechanisms. Accordingly, the present review may serve as a guide for researchers studying the involvement of miR-33a in diverse cancer settings. Contents 1. Introduction 2. miR-33a and its role in cancer 3. Discussion 4. Conclusions

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Suppression of SIRT6 by miR-33a facilitates tumor growth of glioma through apoptosis and oxidative stress resistance

Cited by 38 publications

References 30 publications

<p>Knockdown of circ-TTBK2 Inhibits Glioma Progression by Regulating miR-1283 and CHD1</p>

<p>Knockdown of circ-TTBK2 Inhibits Glioma Progression by Regulating miR-1283 and CHD1</p>

Pharmacological activation of SIRT6 triggers lethal autophagy in human cancer cells

Role of microRNA‑33a in malignant cells (Review)

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