Downstream targets of altered sphingolipid metabolism in response to inhibition of ENOX2 by phenoxodiol

Luca, Thomas De; Bosneaga, Elena; Morré, Dorothy M.; Morré, D. James

doi:10.1002/biof.5520340310

Cited by 12 publications

(4 citation statements)

References 27 publications

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“…We hypothesised that combining a tumour-specific radiation sensitiser with LuPSMA-617 would reduce radiation resistance, prolonging and deepening treatment responses compared with LuPSMA-617 alone. We proposed that idronoxil, via its effects on apoptosis, cell cycle arrest, and topoisomerase II, may impair DNA repair mechanisms and improve sensitivity to LuPSMA-617 [9,10,26]. Furthermore, we postulated 9) 0 (0) 11 (34) Pneumonitis a 0 (0) 1 ( 3) 0 (0) 1 (3) Neutropenia 3 ( 9) 0 (0) 0 (0) 3 ( 9) AE = adverse event.…”

Section: Discussionmentioning

confidence: 99%

“…Idronoxil is a synthetic flavonoid derivative of genistein that inhibits external NADH oxidase 2 (ENOX2) to induce apoptosis and cell cycle arrest, and inhibit DNA topoisomerase 2 [5][6][7][8][9][10]. ENOX2 inhibition activates the sphingomyelinase pathway and deactivates the antiapoptotic protein kinase B (Akt) pathway [10], a key driver of radiotherapy resistance [11]. The targeted effect on ENOX2 has the potential to limit toxicity to noncancer cells, which preferentially express ENOX1 [12].…”

Section: Introductionmentioning

confidence: 99%

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Phase I/II Trial of the Combination of 177Lutetium Prostate specific Membrane Antigen 617 and Idronoxil (NOX66) in Men with End-stage Metastatic Castration-resistant Prostate Cancer (LuPIN)

Crumbaker

Pathmanandavel

Yam

et al. 2021

European Urology Oncology

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Background: Trials of lutetium prostate specific membrane antigen (PSMA) in men with metastatic castration-resistant prostate cancer (mCRPC) have demonstrated good safety and efficacy, but combination strategies may improve outcomes. Idronoxil is a synthetic flavonoid derivative with radiosensitising properties. Objective: To evaluate the safety and activity of 177 Lu PSMA 617 (LuPSMA-617) in combination with idronoxil suppositories (NOX66) in patients with end-stage mCRPC. Design, setting, and participants: Thirty-two men with progressive mCRPC previously treated with taxane-based chemotherapy (91% treated with both docetaxel and cabazitaxel) and abiraterone and/or enzalutamide were enrolled in this phase I dose escalation study with phase II dose expansion. Intervention: Screening with 68 Ga PSMA and 18 F-fludeoxyglucose positron emission tomography (PET)/computed tomography (CT) was performed. Men received up to six cycles of LuPSMA-617 (7.5 GBq) on day 1, with escalating doses of NOX66 on days 1-10 of a 6-wk cycle. Cohort 1 (n = 8) received 400 mg and cohort 2 (n = 24) 800 mg of NOX66. Outcome measurements and statistical analysis: Adverse events (AEs), pain inventory scores, prostate-specific antigen (PSA) response, progression-free survival, and overall survival were evaluated. Results and limitations: Fifty-six men were screened and 32 (57%) were enrolled with a screen failure rate of 21% for PET imaging criteria. Dosing was as follows: 97% (31/32) received two or more doses and 47% (15/32) completed six doses. Common

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Phase I/II Trial of the Combination of 177Lutetium Prostate specific Membrane Antigen 617 and Idronoxil (NOX66) in Men with End-stage Metastatic Castration-resistant Prostate Cancer (LuPIN)

Crumbaker

Pathmanandavel

Yam

et al. 2021

European Urology Oncology

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“…Drug-induced ceramide accumulation inhibits proliferation, induces apoptosis and promotes differentiation [Geilen et al, 1997]. The results with okadaic acid [De Luca et al, 2009] support the concept that ceramide might block activation of Akt by inhibiting its translocation to the cell membrane [Stratford et al, 2001] rather than by promoting its dephosphorylation by phosphatases. Furthermore, an increase in longchain C16-ceramide, the most abundant species produced by SMase activation at the plasma membrane may contribute to the degradation of XIAP and FLIP by activating the proteosome [Kroesen et al, 2003].…”

Section: Discussionmentioning

confidence: 83%

Reciprocal Relationship Between Cytosolic NADH and ENOX2 Inhibition Triggers Sphingolipid‐Induced Apoptosis in HeLa Cells

Luca

Morré

2010

J of Cellular Biochemistry

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ENOX2 (tNOX), a tumor-associated cell surface ubiquinol (NADH) oxidase, functions as an alternative terminal oxidase for plasma membrane electron transport. Ubiquitous in all cancer cell lines studied thus far, ENOX2 expression correlates with the abnormal growth and division associated with the malignant phenotype. ENOX2 has been proposed as the cellular target for various quinone site inhibitors that demonstrate anticancer activity such as the green tea constituent epigallocatechin-3-gallate (EGCg) and the isoflavone phenoxodiol (PXD). Here we present a possible mechanism that explains how these substances result in apoptosis in cancer cells by ENOX2-mediated alterations of cytosolic amounts of NAD(+) and NADH. When ENOX2 is inhibited, plasma membrane electron transport is diminished, and cytosolic NADH accumulates. We show in HeLa cells that NADH levels modulate the activities of two pivotal enzymes of sphingolipid metabolism: sphingosine kinase 1 (SK1) and neutral sphingomyelinase (nSMase). Their respective products sphingosine 1-phosphate (S1P) and ceramide (Cer) are key determinants of cell fate. S1P promotes cell survival and Cer promotes apoptosis. Using plasma membranes isolated from cervical adenocarcinoma (HeLa) cells as well as purified proteins of both bacterial and human origin, we demonstrate that NADH inhibits SK1 and stimulates nSMase, while NAD(+) inhibits nSMase and has no effect on SK1. Additionally, intact HeLa cells treated with ENOX2 inhibitors exhibit an increase in Cer and a decrease in S1P. Treatments that stimulate cytosolic NADH production potentiate the antiproliferative effects of ENOX2 inhibitors while those that attenuate NADH production or stimulate plasma membrane electron transport confer a survival advantage.

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“…Mouse embryonic fibroblasts derived from transgenic mice overexpressing a truncated form of ENOX2 showed accelerated growth rates with respect to wild-type fibroblasts and enhanced invasiveness (315). In contrast, decreased cell growth and migration, as well as increased cell death, are observed when the function of ENOX2 is impaired, either by inhibiting the catalytic activity with (3)-epigallocatechin-3-gallate, capsaicin, phenoxodiol, or anti-ENOX2 antibodies (47,72,306,315) or by down-modulating its expression by RNA interference (173). Morré and colleagues also viewed ENOX2 as both (i) a noninvasive, circulating tumor marker (based on their description of several cancer-type specific ENOX2 isoforms) (119,307) and (ii) a potential antitumoral drug target, since this enzyme is blocked by quinone site inhibitors, which also exhibit anticancer activity (54,119,208).…”

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confidence: 89%

Trans-Plasma Membrane Electron Transport in Mammals: Functional Significance in Health and Disease

Principe

Avigliano

Savini

et al. 2011

Antioxidants & Redox Signaling

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Trans-plasma membrane electron transport (t-PMET) has been established since the 1960s, but it has only been subject to more intensive research in the last decade. The discovery and characterization at the molecular level of its novel components has increased our understanding of how t-PMET regulates distinct cellular functions. This review will give an update on t-PMET, with particular emphasis on how its malfunction relates to some diseases, such as cancer, abnormal cell death, cardiovascular diseases, aging, obesity, neurodegenerative diseases, pulmonary fibrosis, asthma, and genetically linked pathologies. Understanding these relationships may provide novel therapeutic approaches for pathologies associated with unbalanced redox state.

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Downstream targets of altered sphingolipid metabolism in response to inhibition of ENOX2 by phenoxodiol

Cited by 12 publications

References 27 publications

Phase I/II Trial of the Combination of 177Lutetium Prostate specific Membrane Antigen 617 and Idronoxil (NOX66) in Men with End-stage Metastatic Castration-resistant Prostate Cancer (LuPIN)

Phase I/II Trial of the Combination of 177Lutetium Prostate specific Membrane Antigen 617 and Idronoxil (NOX66) in Men with End-stage Metastatic Castration-resistant Prostate Cancer (LuPIN)

Reciprocal Relationship Between Cytosolic NADH and ENOX2 Inhibition Triggers Sphingolipid‐Induced Apoptosis in HeLa Cells

Trans-Plasma Membrane Electron Transport in Mammals: Functional Significance in Health and Disease

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