Glucose metabolism and NRF2 coordinate the antioxidant response in melanoma resistant to MAPK inhibitors

Khamari, Raeeka; Trinh, Anne; Gabert, Pierre Elliott; Corazao-Rozas, Paola; Riveros-Cruz, Samuel; Balayssac, Stéphane; Malet‐Martino, Myriam; Dekiouk, Salim; Curt, Marie Joncquel Chevalier; Maboudou, Patrice; Garçon, Guillaume; Ravasi, Laura; Guerreschi, P.; Mortier, Laurent; Quesnel, Bruno; Marchetti, Philippe; Kluza, Jérôme

doi:10.1038/s41419-018-0340-4

Cited by 64 publications

(75 citation statements)

References 37 publications

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“…Here, A375RIV1 cells exhibited a strong activation of the NRF2 signaling, followed by an increased expression of genes involved in ROS scavenging (i.e., GPX1, GPX2), GSH synthesis (i.e., GCLM, and xCT) and NADPH-generation (i.e., TKT, TALDO1), compared to the A375-v counterpart. Of note, NRF2 KD by siRNA decreased the protein content of its target genes in A375RIV1 cells, partly reversing their resistance to Vemurafenib [253]. Thus, the xCT system is key regulator of cancer cells redox balance, while its inactivation might sensitize malignant cells to OS inducers.…”

Section: Nrf2 Regulates Metabolic Processes Leading To Gsh Synthesis mentioning

confidence: 97%

Potential Applications of NRF2 Modulators in Cancer Therapy

et al. 2020

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The nuclear factor erythroid 2-related factor 2 (NRF2)–Kelch-like ECH-associated protein 1 (KEAP1) regulatory pathway plays an essential role in protecting cells and tissues from oxidative, electrophilic, and xenobiotic stress. By controlling the transactivation of over 500 cytoprotective genes, the NRF2 transcription factor has been implicated in the physiopathology of several human diseases, including cancer. In this respect, accumulating evidence indicates that NRF2 can act as a double-edged sword, being able to mediate tumor suppressive or pro-oncogenic functions, depending on the specific biological context of its activation. Thus, a better understanding of the mechanisms that control NRF2 functions and the most appropriate context of its activation is a prerequisite for the development of effective therapeutic strategies based on NRF2 modulation. In line of principle, the controlled activation of NRF2 might reduce the risk of cancer initiation and development in normal cells by scavenging reactive-oxygen species (ROS) and by preventing genomic instability through decreased DNA damage. In contrast however, already transformed cells with constitutive or prolonged activation of NRF2 signaling might represent a major clinical hurdle and exhibit an aggressive phenotype characterized by therapy resistance and unfavorable prognosis, requiring the use of NRF2 inhibitors. In this review, we will focus on the dual roles of the NRF2-KEAP1 pathway in cancer promotion and inhibition, describing the mechanisms of its activation and potential therapeutic strategies based on the use of context-specific modulation of NRF2.

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Section: Nrf2 Regulates Metabolic Processes Leading To Gsh Synthesis mentioning

confidence: 97%

Potential Applications of NRF2 Modulators in Cancer Therapy

et al. 2020

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“…4A, 4B). The transcrip-tion factor NRF2 is known to coordinate antioxidant responses in cells and mediates MAPK inhibitor resistance in melanoma cells (20,35). Although not successfully identified by proteome profiling, we performed immunofluorescence staining and detected positive signals in all investigated melanoma cells (Fig.…”

Section: Eicosanoid Formation In Metastatic Variants-besidesmentioning

confidence: 99%

The Challenge of Classifying Metastatic Cell Properties by Molecular Profiling Exemplified with Cutaneous Melanoma Cells and Their Cerebral Metastasis from Patient Derived Mouse Xenografts

Neuditschko

Janker²,

Niederstaetter³

et al. 2020

Molecular & Cellular Proteomics

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The prediction of metastatic properties from molecular analyses still poses a major challenge. Here we aimed at the classification of metastasis-related cell properties by proteome profiling making use of cutaneous and brain-metastasizing variants from single melanomas sharing the same genetic ancestry. Previous experiments demonstrated that cultured cells derived from these xenografted variants maintain a stable phenotype associated with a differential metastatic behavior: The brain metastasizing variants produce more spontaneous micro-metastases than the corresponding cutaneous variants. Four corresponding pairs of cutaneous and metastatic cells were obtained from four individual patients, resulting in eight cell-lines presently investigated. Label free proteome profiling revealed significant differences between corresponding pairs of cutaneous and cerebellar metastases from the same patient. Indeed, each brain metastasizing variant expressed several apparently metastasis-associated proteomic alterations as compared with the corresponding cutaneous variant. Among the differentially expressed proteins we identified cell adhesion molecules, immune regulators, epithelial to mesenchymal transition markers, stem cell markers, redox regulators and cytokines. Similar results were observed regarding eicosanoids, considered relevant for metastasis, such as PGE2 and 12-HETE. Multiparametric morphological analysis of cells also revealed no characteristic alterations associated with the cutaneous and brain metastasis variants. However, no correct classification regarding metastatic potential was yet possible with the present data. We thus concluded that molecular profiling is able to classify cells according to known functional categories but is not yet able to predict relevant cell properties emerging from networks consisting of many interconnected molecules. The presently observed broad diversity of molecular patterns, irrespective of restricting to one tumor type and two main classes of metastasis, highlights the important need to develop meta-analysis strategies to predict cell properties from molecular profiling data. Such base knowledge will greatly support future individualized precision medicine approaches.

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“…Indeed, we show that the disruption of this redox buffer improves the outcomes of targeted therapies. In summary, our findings suggest that modulation of cancer antioxidant defense could be exploited to augment the benefits of existing therapies in melanoma (Khamari et al, 2018;Yuan et al, 2018) . This strategy may extend beyond melanoma, as antioxidant pathways have been implicated in tumor progression, and drug resistance (Harris et al, 2015;Ji et al, 2018;Sarmiento-Salinas et al, 2019) .…”

Section: Discussionmentioning

confidence: 80%

“…The link between oxidative stress and drug response in melanoma is beginning to be explored Zaal and Berkers, 2018) . BRAF-inhibitor resistant melanomas were shown to upregulate NRF2 -mediated antioxidant response to maintain cell survival (Khamari et al, 2018) . Nonetheless, it still remains to be examined how redox potential of melanoma cells affects their drug sensitivity, and how it is maintained under BRAF-inhibition.…”

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confidence: 99%

Disruption of Redox Balance Enhances the Effects of BRAF-inhibition in Melanoma Cells

Paudel

et al. 2019

Preprint

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Melanomas harboring BRAF mutations can be treated with BRAF inhibitors (BRAFi), but responses are varied and tumor recurrence is inevitable. Here, using an integrative approach of experimentation and mathematical flux balance analyses in BRAF -mutated melanoma cells, we report that elevated antioxidant capacity is linked to BRAFi sensitivity in melanoma cells. High levels of antioxidant metabolites in cells with reduced BRAFi sensitivity confirm this conclusion. By extending our analyses to other melanoma subtypes in TCGA, we predict that elevated redox capacity is a general feature of melanomas, not previously observed. We propose that redox vulnerabilities could be exploited for therapeutic benefits and identify unsuspected combination targets to enhance the effects of BRAFi in any melanoma, regardless of mutational status.

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Glucose metabolism and NRF2 coordinate the antioxidant response in melanoma resistant to MAPK inhibitors

Cited by 64 publications

References 37 publications

Potential Applications of NRF2 Modulators in Cancer Therapy

Potential Applications of NRF2 Modulators in Cancer Therapy

The Challenge of Classifying Metastatic Cell Properties by Molecular Profiling Exemplified with Cutaneous Melanoma Cells and Their Cerebral Metastasis from Patient Derived Mouse Xenografts

Disruption of Redox Balance Enhances the Effects of BRAF-inhibition in Melanoma Cells

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