Metformin in combination with JS-K inhibits growth of renal cell carcinoma cells via reactive oxygen species activation and inducing DNA breaks

Zhao, Yuwan; Luo, Qiuming; Mo, Jierong; Li, Jianwei; Ye, Dongcai; Ao, Zhixian; Chen, Lixin; Liu, Jianjun

doi:10.7150/jca.36372

Cited by 17 publications

(7 citation statements)

References 41 publications

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“…We speculated that synergistic killing-effect in our study was due to Met providing ROS or RNS to CAP, enhancing the CAP-associated cell death. Although Met has been reported as an antioxidant regent in diabetic patients [36], there was research suggested Met increased intracellular ROS [37]. The radical (OH or O 2 -) induced oxidation byproducts of metformin did not contain ROS and RNS [38], this means that the interaction between CAP and Met may not contribute to the synergistically inhibitory effect.…”

Section: Discussionmentioning

confidence: 97%

Combination of metformin and cold atmospheric plasma induces glioma cell death to associate with c-Fos

Yang

Zhou

Hai-yan

et al. 2021

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Glioma is the most common type of brain cancer. Chemotherapy combination with surgery and radiotherapy is a standard treatment for patients. Although there are many advances in glioma therapy, the prognosis of glioma patients has not significantly been improved over the past decades. Hence, there is still an urgent need to develop a new therapy to treat glioma. Cell viability was assessed by CellTiter Blue assay; flow cytometry (FCM) was used for detecting cell apoptosis; ROS detection was detected by ROS Assay; H 2 O 2 detection was performed by hydrogen peroxide detection kits; real-time PCR and WB were used to determine gene expression. Using the glioma cell line U251 and U87, we investigated a possible combination inhibitory effect includes metformin and cold atmospheric plasma (CAP). The combinatio n treatment showed a synergistic inhibitory effect on cell viability, significantly inducing cell apoptosis. Furthermore, we also found H 2 O 2 produced by CAP has an important role in the synergistic inhibitory effect, eliminating H 2 O 2 with catalase reversed the synergistic inhibitory effect. In addition, the transcript and protein levels of c-FOS were robustly increased after co-treated with metformin and CAP. Taken together, we propose that pre-treatment glioma cells with metformin sensitize tumor cells to CAP, which may serve as a potential therapeutic strategy for glioma.

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Section: Discussionmentioning

confidence: 97%

Combination of metformin and cold atmospheric plasma induces glioma cell death to associate with c-Fos

Yang

Zhou

Hai-yan

et al. 2021

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“…In colon cancer cells, the antidiabetic drug, combined with cisplatin, inhibited cell viability, decreased colony formation, and induced the intrinsic apoptosis pathway through increased ROS-mediated PI3K/Akt signaling pathway activity [302]. In lung cancer cells, by means of in vitro and in vivo studies, it has been shown that metformin, in combination with celecoxib, induces ROS aggregation, leading to mitochondrial membrane potential alteration, DNA double-strand breaks and increased expression of the tumor suppressor factor p53, causing cell cycle arrest and cell proliferation inhibition [303]; similar mechanisms were reported to mediate the antitumor activity of metformin, in combination with standard therapies, in different types of cancer cells [304][305][306][307].…”

Section: Targeting Mitochondrial Functional and Structural Dynamicsmentioning

confidence: 90%

The multifaceted roles of mitochondria at the crossroads of cell life and death in cancer

Fontana

Limonta

2021

Free Radical Biology and Medicine

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“…Metformin was already shown to successfully prevent cancer cell viability and cell proliferation by inducing G 2 /M cell cycle arrest in a dose and time-dependent fashion followed by programmed cell death induction, effects that were attributed to increased ROS levels [68]. Likewise metformin targeted mitochondria-dependent apoptosis, and inducing DNA breaks by activating ROS [71]. Moreover, ROS levels vary during cell cycle progression and peak in mitosis.…”

Section: Discussionmentioning

confidence: 99%

Metformin Protects against Radiation-Induced Acute Effects by Limiting Senescence of Bronchial-Epithelial Cells

Hansel

Barr

Schemann

et al. 2021

IJMS

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Radiation-induced damage to normal lung parenchyma remains a dose-limiting factor in thorax-associated radiotherapy (RT). Severe early and late complications with lungs can increase the risk of morbidity in cancer patients after RT. Herein, senescence of lung epithelial cells following RT-induced cellular stress, or more precisely the respective altered secretory profile, the senescence-associated secretory phenotype (SASP), was suggested as a central process for the initiation and progression of pneumonitis and pulmonary fibrosis. We previously reported that abrogation of certain aspects of the secretome of senescent lung cells, in particular, signaling inhibition of the SASP-factor Ccl2/Mcp1 mediated radioprotection especially by limiting endothelial dysfunction. Here, we investigated the therapeutic potential of a combined metformin treatment to protect normal lung tissue from RT-induced senescence and associated lung injury using a preclinical mouse model of radiation-induced pneumopathy. Metformin treatment efficiently limited RT-induced senescence and SASP expression levels, thereby limiting vascular dysfunctions, namely increased vascular permeability associated with increased extravasation of circulating immune and tumor cells early after irradiation (acute effects). Complementary in vitro studies using normal lung epithelial cell lines confirmed the senescence-limiting effect of metformin following RT finally resulting in radioprotection, while fostering RT-induced cellular stress of cultured malignant epithelial cells accounting for radiosensitization. The radioprotective action of metformin for normal lung tissue without simultaneous protection or preferable radiosensitization of tumor tissue might increase tumor control probabilities and survival because higher radiation doses could be used.

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Metformin in combination with JS-K inhibits growth of renal cell carcinoma cells via reactive oxygen species activation and inducing DNA breaks

Cited by 17 publications

References 41 publications

Combination of metformin and cold atmospheric plasma induces glioma cell death to associate with c-Fos

Combination of metformin and cold atmospheric plasma induces glioma cell death to associate with c-Fos

The multifaceted roles of mitochondria at the crossroads of cell life and death in cancer

Metformin Protects against Radiation-Induced Acute Effects by Limiting Senescence of Bronchial-Epithelial Cells

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