Inhibition of Na+/K+-ATPase induces hybrid cell death and enhanced sensitivity to chemotherapy in human glioblastoma cells

Chen, Dongdong; Song, Mingke; Mohamad, Osama; Yu, Shan Ping

doi:10.1186/1471-2407-14-716

Cited by 77 publications

(72 citation statements)

References 59 publications

(75 reference statements)

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“…These results are in accordance with previous genetic studies showing high prevalence of mutations in ion channel genes in tissue samples from patients with GBM . However, other studies using in vitro glioma cell lines suggested enhanced sensitivity of glioma cells to chemotherapy following treatment with digoxin or amiodarone . Among the biological mechanisms proposed for this protective effect were inhibition of tumor invasion and migration through effects on cellular volume and shape, induction of apoptosis through cellular hyperpolarization and reduced secretion of the tumor promoting vascular endothelial growth factor.…”

Section: Discussionsupporting

confidence: 91%

Ion channel blockers and glioblastoma risk and outcome: a nested case–control and retrospective cohort studies

Boursi

Han

Haynes

et al. 2016

Pharmacoepidemiology and Drug

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Purpose Mutations in ion-channels are common among patients with glioblastoma multiforme (GBM) and promote cell migration and invasion. We sought to evaluate the association between the use of specific ion-channel blockers such as digoxin, amiodarone, diltiazem and verapamil and GBM risk and survival. Methods We conducted a nested case-control study in a large primary care database from the UK. Cases were defined as all individuals with incident diagnosis of GBM during follow-up. For each case, up to four controls were selected using incidence-density sampling. The primary exposure of interest was active treatment with each of the four ion-channel blockers. We used conditional logistic regression to estimate odds-ratios (ORs) and 95% confidence-interval (CI) for the association between ion-channel blocker use and GBM risk. We then performed a Cox regression analysis among those diagnosed with GBM in order to evaluate the association between use of ion-channel blockers and overall survival. Both analyses were adjusted to common confounders. Results The study included 1,076 cases and 4,253 matched controls. There was no statistically significant difference between cases and controls in cardiac and metabolic risk factors. There was no change in GBM risk in active users of ion-channel blockers compared to non-users. Among patients with GBM, active users of amiodarone had worse survival compared to never users with an HR of 4.41 (95%CI 1.95-9.96). There was no statistically significant change in survival among diltiazem, verapamil or digoxin users. Conclusion Treatment with specific ion-channel blockers was not associated with the risk of GBM, but was associated with worse survival in GBM patients.

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Section: Discussionsupporting

confidence: 91%

Ion channel blockers and glioblastoma risk and outcome: a nested case–control and retrospective cohort studies

Boursi

Han

Haynes

et al. 2016

Pharmacoepidemiology and Drug

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“…Recently, many investigations demonstrated the important role of α-1 Na inhibitors in prostate cancer cell is inhibition of ɑ1-subunit so it consequently suppresses proliferation and migration of cancer cell and reduce metastasis of tumor (Chen et al, 2014). Therefore, this work plan targeted to determine α-1 Na…”

Section: Effect Of Vitex Berries Extract On Rate Limiting Enzymes Andmentioning

confidence: 99%

Protective and therapeutic effect of Vitex agnus-castus against prostate cancer in rat

2017

J App Pharm Sci

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This work was prompted to investigate effect of the vitex berries crude extract on prostate cancer relevant to the cancer growth rate limiting enzymes (5-α reductase and Na + /K + ATPase, tumor biomarker; prostate specific antigen (PSA), carcinoembryonic antigen (CEA), sexual hormones; testosterone and luteinizing hormone, antiinflammatory markers and antioxidant markers. Vitex berries crude extract was prepared and tested against human prostate cancer cell line (PC3) and then incorporated into in-vivo model for prostate cancer induced chemically in rats using chronic administration of testosterone (3mg/ kg/ 90 days) in a sub-cutaneous route and intraperitoneal injection of carcinogenic material, 7,12-Dimethylbenz(a)anthracene (DMBA) at dose of 65 mg/kg as a single dose. Vitex extract at dose of 165 mg/kg/day inhibited cell growth of PC3 which were completely killed at 100μg/ml. In in-vivo study, Vitex extract showed potent anti-prostate cancer evident as significant reduction in cancer growth rate limiting enzymes; 5-α reductase, Na + /K + ATPase and prostate specific antigen with suppression in carcinoembryonic antigen production, which amplified by prostate cancer induction. A selective anti-inflammatory effect was recorded with vitex administration represented as significant inhibition in cyclooxygenase-2 and non-significant effect on cyclooxygenase-1. It showed ameliorative effects on sexual hormones showed in amendment in testosterone and luteinizing hormone affected by prostate cancer induction. Investigations of this work prove vitex extract has potential role as anti-prostate cancer evaluated by in-vitro and in-vivo protocols. The anti-prostate cancer properties of vitex extract may be due to its effect against cancer risk factors; antioxidant and anti-inflammatory characters, ameliorative effect on sex hormones and suppression in cancer growth rate limiting enzymes.

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“…There have been a number of studies to suggest that the Na + /K + -ATPase is upregulated in malignant cancers, including gliomas (Sakai et al 2004; Mijatovic et al 2006; Klatte et al 2008; Lefranc et al 2008; Mathieu et al 2009). In gliomas, the Na + /K + -ATPase α1 subunit, which is responsible for the exchange of Na + for K + , has been found to be upregulated and localized to the plasma membrane (Lefranc et al 2008; Chen et al 2014). It is unclear, however, what effect this upregulation is playing in glioma biology.…”

Section: Transporters That Establish and Maintain Ionic Gradientsmentioning

confidence: 99%

A role for ion channels in perivascular glioma invasion

Thompson

Sontheimer

2016

Eur Biophys J

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Malignant gliomas are devastating tumors, frequently killing those diagnosed in little over a year. The profuse infiltration of glioma cells into healthy tissue surrounding the main tumor mass is one of the major obstacles limiting the improvement of patient survival. Migration along the abluminal side of blood vessels is one of the salient features of glioma cell invasion. Invading glioma cells are attracted to the vascular network, in part by the neuro-peptide bradykinin, where glioma cells actively modify the gliovascular interface and undergo volumetric alterations to navigate the confined space. Critical to these volume modifications is a proposed hydrodynamic model that involves the flux of ions in and out of the cell, followed by osmotically obligated water. Ion and water channels expressed by the glioma cell are essential in this model of invasion and make opportune therapeutic targets. Lastly, there is growing evidence that vascular-associated glioma cells are able to control the vascular tone, presumably to free up space for invasion and growth. The unique mechanisms that enable perivascular glioma invasion may offer critical targets for therapeutic intervention in this devastating disease. Indeed, a chloride channel-blocking peptide has already been successfully tested in human clinical trials.

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Inhibition of Na+/K+-ATPase induces hybrid cell death and enhanced sensitivity to chemotherapy in human glioblastoma cells

Cited by 77 publications

References 59 publications

Ion channel blockers and glioblastoma risk and outcome: a nested case–control and retrospective cohort studies

Ion channel blockers and glioblastoma risk and outcome: a nested case–control and retrospective cohort studies

Protective and therapeutic effect of Vitex agnus-castus against prostate cancer in rat

A role for ion channels in perivascular glioma invasion

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