SIRT1 Regulates the Chemoresistance and Invasiveness of Ovarian Carcinoma Cells

Mvunta, David Hamisi; Miyamoto, Tsutomu; Asaka, Ryoichi; Yumura, Yasushi; Ando, Hirofumi; Higuchi, Satoshi; Ito, Koichi; Kashima, Hiroyasu; Shiozawa, Tanri

doi:10.1016/j.tranon.2017.05.005

Cited by 36 publications

(38 citation statements)

References 41 publications

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“…Conversely, over-expression of SIRT1 was frequently observed in all kinds of non-melanoma skin cancers, including squamous cell carcinoma, basal cell carcinoma, Bowen's disease, and actinic keratosis [41,42]. Additionally, expression of SIRT1 was more strongly expressed in OVCA3 cells than in immortalized ovarian surface epithelium OSE7E cells [43]. In particular, over-expression of SIRT1 is correlated with lymph node metastasis and the decrease of the 5-year survival rate, indicating its oncogenic effects in ovarian cancer [40,42].…”

Section: Discussionmentioning

confidence: 97%

A new SIRT1 inhibitor, MHY2245, induces autophagy and inhibits energy metabolism via PKM2/mTOR pathway in human ovarian cancer cells

Tae¹,

Son²,

Lee³

et al. 2020

Int. J. Biol. Sci.

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Ovarian cancer is a common gynecological cancer that is found worldwide. Class III histone deacetylase (HDAC) inhibitors, a new class of anticancer agents, induce autophagy in various human cancer cells. The aim of the present study was to investigate the antitumor activity of MHY2245, a new synthetic SIRT inhibitor, on human ovarian cancer cells. We found that MHY2245 exhibited potent cytotoxicity to SKOV3 cells in a time-and concentration-dependent manner. The cytotoxicity of MHY2245 (IC 50 =0.32 µM) was higher than that of doxorubicin (DOX, IC 50 =1.38µM) against SKOV3 cells. MHY2245 significantly inhibited SIRT1 enzyme activity, reduced the expression of SIRT1, increased cell cycle arrest at G 2 /M phase, and induced apoptotic cell death in SKOV3 cells via expression of cytochrome c, cleaved-PARP, cleaved caspase-3, and Bax. This might be associated with blocking of the pyruvate kinase M2 (PKM2)/mTOR pathway. MHY2245 also inhibited tumor growth and reduced tumor size when SKOV3 cells were transplanted into nude mice. Our results indicate that MHY2245 exerts antitumor activity against ovarian cancer cells by blocking the PKM2/mTOR pathway. We suggest that MHY2245 is a promising anticancer agent that disrupts ovarian cancer cell metabolism.

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Section: Discussionmentioning

confidence: 97%

A new SIRT1 inhibitor, MHY2245, induces autophagy and inhibits energy metabolism via PKM2/mTOR pathway in human ovarian cancer cells

Tae¹,

Son²,

Lee³

et al. 2020

Int. J. Biol. Sci.

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“…Because overexpression of SIRT1 reportedly renders cancer cells resistant to anti-cancer drugs [18,19], we examined SIRT1 levels in multidrug-resistant LS513 cells. ActD upregulated SIRT1 expression while Rp1 attenuated this effect to enhance cell death, as determined by increased PARP cleavage (Figure 2A).…”

Section: Rp1 Attenuates Actd-induced Sirt1 Upregulationmentioning

confidence: 99%

Ginsenoside Rp1, A Ginsenoside Derivative, Augments Anti-Cancer Effects of Actinomycin D via Downregulation of an AKT-SIRT1 Pathway

Yun

Lee

et al. 2020

Cancers

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Novel strategies for overcoming multidrug resistance are urgently needed to improve chemotherapy success and reduce side effects. Ginsenosides, the main active components of Panax ginseng, display anti-cancer properties and reverse drug resistance; however, the biological pathways mediating this phenomenon remain incompletely understood. This study aimed to evaluate the anti-cancer effects of ginsenoside Rp1, actinomycin D (ActD), and their co-administration in drug-resistant cells and murine xenograft model of colon cancer, and explore the underlying mechanisms. ActD increased expression and activity of SIRT1 in drug-resistant LS513 colon cancer, OVCAR8-DXR ovarian cancer, and A549-DXR lung cancer cells, but not in ActD-sensitive SW620 colon cancer cells. Inhibition of SIRT1, either pharmacologically, with EX527 or through siRNA, stimulated p53 acetylation and apoptosis in LS513 cells when treated with ActD. ActD also increased AKT activation in drug-resistant cells. Inhibition of AKT abrogated ActD-induced upregulation of SIRT1, suggesting that the AKT-SIRT1 pathway is important in ActD resistance. Rp1 inhibited both ActD-induced AKT activation and SIRT1 upregulation and re-sensitized the cells to ActD. Synergistic antitumor effects of Rp1 with ActD were also observed in vivo. Our results suggest that combining Rp1 with chemotherapeutic agents could circumvent drug resistance and improve treatment efficacy.

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“…Twelve known compounds were identified as perlolyrin (4) [8,9], 3-(9H-β-carbolin-1-yl)acrylic acid methyl ester (5) [8,9] [19][20][21]. However, SIRT1 is also a double-edged sword exemplified by tumor, it functions as an oncogene as well as a tumor suppressor [22]. Considering the traditional medicinal uses of the roots of C. pilosula and the roels of SIRT1 activation in energy metabolism [23], all the isolates were therefore examined for their regulatory activity on SIRT1.…”

mentioning

confidence: 99%

Compounds from the Roots of Codonopsis pilosula and Their SIRT1 Regulatory Activity

Zheng

Cheng

Yan

et al. 2018

Natural Product Communications

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Two new compounds, pilosuloside A (1) and pilosulain A (2), one new natural occurring compound (3), and twelve known compounds (4-15), were isolated from the roots of Codonopsis pilosula. Their structures were elucidated by a combination of spectroscopic methods. Regulation of SIRT1 activity by all the compounds was evaluated. The results showed that 4 could activate SIRT1 in a concentration-dependent manner.

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SIRT1 Regulates the Chemoresistance and Invasiveness of Ovarian Carcinoma Cells

Cited by 36 publications

References 41 publications

A new SIRT1 inhibitor, MHY2245, induces autophagy and inhibits energy metabolism via PKM2/mTOR pathway in human ovarian cancer cells

A new SIRT1 inhibitor, MHY2245, induces autophagy and inhibits energy metabolism via PKM2/mTOR pathway in human ovarian cancer cells

Ginsenoside Rp1, A Ginsenoside Derivative, Augments Anti-Cancer Effects of Actinomycin D via Downregulation of an AKT-SIRT1 Pathway

Compounds from the Roots of Codonopsis pilosula and Their SIRT1 Regulatory Activity

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