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6 results on '"Mourah, Samia"'

1. Supplementary Figures for Novel treatment strategy for NRAS-mutated melanoma through a selective inhibitor of CD147/VEGFR-2 interaction

Author

Fernández-Recio, Juan [0000-0002-3986-7686], Landras, Alexandra, Reger De Moura, Coralie, Villoutreix, Bruno O., Battistella, Maxime, Sadoux, Aurélie, Dumaz, Nicolas, Menash, Suzanne, Fernández-Recio, Juan, Lebbe, Céleste, Mourah, Samia, Fernández-Recio, Juan [0000-0002-3986-7686], Landras, Alexandra, Reger De Moura, Coralie, Villoutreix, Bruno O., Battistella, Maxime, Sadoux, Aurélie, Dumaz, Nicolas, Menash, Suzanne, Fernández-Recio, Juan, Lebbe, Céleste, and Mourah, Samia

Abstract

This PDF file includes: Supplementary Figures. S1 to S11

Published
2022

2. Supplementary Materials and Methods for Novel treatment strategy for NRAS-mutated melanoma through a selective inhibitor of CD147/VEGFR-2 interaction

Author

Fernández-Recio, Juan [0000-0002-3986-7686], Landras, Alexandra, Reger De Moura, Coralie, Villoutreix, Bruno O., Battistella, Maxime, Sadoux, Aurélie, Dumaz, Nicolas, Menash, Suzanne, Fernández-Recio, Juan, Lebbe, Céleste, Mourah, Samia, Fernández-Recio, Juan [0000-0002-3986-7686], Landras, Alexandra, Reger De Moura, Coralie, Villoutreix, Bruno O., Battistella, Maxime, Sadoux, Aurélie, Dumaz, Nicolas, Menash, Suzanne, Fernández-Recio, Juan, Lebbe, Céleste, and Mourah, Samia

Abstract

This PDF file includes: Supplementary Materials and Methods

Published
2022

3. Novel treatment strategy for NRAS-mutated melanoma through a selective inhibitor of CD147/VEGFR-2 interaction

Author

Ligue Nationale contre le Cancer (France), Institut National de la Santé et de la Recherche Médicale (France), Société Française de Dermatologie, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Landras, Alexandra, Reger De Moura, Coralie, Villoutreix, Bruno O., Battistella, Maxime, Sadoux, Aurélie, Dumaz, Nicolas, Menash, Suzanne, Fernández-Recio, Juan, Lebbe, Céleste, Mourah, Samia, Ligue Nationale contre le Cancer (France), Institut National de la Santé et de la Recherche Médicale (France), Société Française de Dermatologie, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Landras, Alexandra, Reger De Moura, Coralie, Villoutreix, Bruno O., Battistella, Maxime, Sadoux, Aurélie, Dumaz, Nicolas, Menash, Suzanne, Fernández-Recio, Juan, Lebbe, Céleste, and Mourah, Samia

Abstract

More than 70% of human NRAS melanomas are resistant to MEK inhibitors highlighting the crucial need for efficient therapeutic strategies for these tumors. CD147, a membrane receptor, is overexpressed in most cancers including melanoma and is associated with poor prognosis. We show here that CD147i, a specific inhibitor of CD147/VEGFR-2 interaction represents a potential therapeutic strategy for NRAS melanoma cells. It significantly inhibited the malignant properties of NRAS melanomas ex vivo and in vivo. Importantly, NRAS patient’s-derived xenografts, which were resistant to MEKi, became sensitive when combined with CD147i leading to decreased proliferation ex vivo and tumor regression in vivo. Mechanistic studies revealed that CD147i effects were mediated through STAT3 pathway. These data bring a proof of concept on the impact of the inhibition of CD147/VEGFR-2 interaction on melanoma progression and represents a new therapeutic opportunity for NRAS melanoma when combined with MEKi.

Published
2022

4. Fgf2 induces resistance to nilotinib through mapk pathway activation in kit mutated melanoma

Author

Tétu, Pauline, Delyon, Julie, André, Jocelyne, De Moura, Coralie Reger, Sabbah, Malak, Ghanem, Ghanem Elias, Batistella, Maxime, Mourah, Samia, Lebbe, Céleste, Dumaz, Nicolas, Tétu, Pauline, Delyon, Julie, André, Jocelyne, De Moura, Coralie Reger, Sabbah, Malak, Ghanem, Ghanem Elias, Batistella, Maxime, Mourah, Samia, Lebbe, Céleste, and Dumaz, Nicolas

Abstract

KIT is a bona fide oncogene in a subset of melanoma and, ex vivo, KIT inhibitors are very efficient at killing KIT-mutant melanoma cell lines. However, KIT-mutant melanoma tumors tend to show a de novo resistance in most cases and a limited duration of response when response is achieved. We performed pharmacodynamic studies on patients with KIT-mutated melanoma treated with nilotinib, which suggested that the FGF2 axis may be a mechanism of resistance in this subset of melanoma. Using several melanoma cell lines, which are dependent on oncogenic KIT, we showed that although KIT inhibition markedly decreased cell viability in melanoma cell lines with distinct KIT mutations, this effect was lessened in the presence of FGF2 due to inhibition of BIM expression by MAPK pathway activation. Addition of a MEK inhibitor reversed the FGF2-driven resistance for all KIT mutants. We confirmed the expression of FGF2 and activation of MEK-ERK in melanoma patients using in situ data from a clinical trial. Therefore, the combined inhibition of KIT with FGFR or MEK may be a next-step effective clinical strategy in KIT-mutant melanoma., SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2020

6. EMMPRIN/CD147 is a novel coreceptor of VEGFR-2 mediating its activation by VEGF

Author

Barcelona Supercomputing Center, Khayati, Farah, Pérez-Cano, Laura, Maouche, Kamel, Sadoux, Aurélie, Boutalbi, Zineb, Podgorniak, Marie-Pierre, Maskos, Uwe, Setterblad, Niclas, Janin, Anne, Calvo, Fabien, Lebbé, Céleste, Menashi, Suzanne, Fernández-Recio, Juan, Mourah, Samia, Barcelona Supercomputing Center, Khayati, Farah, Pérez-Cano, Laura, Maouche, Kamel, Sadoux, Aurélie, Boutalbi, Zineb, Podgorniak, Marie-Pierre, Maskos, Uwe, Setterblad, Niclas, Janin, Anne, Calvo, Fabien, Lebbé, Céleste, Menashi, Suzanne, Fernández-Recio, Juan, and Mourah, Samia

Abstract

EMMPRIN/CD147 is mainly known for its protease inducing function but a role in promoting tumor angiogenesis has also been demonstrated. This study provides evidence that EMMPRIN is a new coreceptor for the VEGFR-2 tyrosine kinase receptor in both endothelial and tumor cells, as it directly interacts with it and regulates its activation by its VEGF ligand, signalling and functional consequences both in vitro and in vivo. Computational docking analyses and mutagenesis studies identified a molecular binding site in the extracellular domain of EMMPRIN located close to the cell membrane and containing the amino acids 195/199. EMMPRIN is overexpressed in cancer and hence is able to further potentiate VEGFR-2 activation, suggesting that a combinatory therapy of an antiangiogenic drug together with an inhibitor of EMMPRIN/VEGFR-2 interaction may have a greater impact on inhibiting angiogenesis and malignancy., This work was supported by Institut National de la Santé et de la Recherche Médicale (INSERM), La Ligue Nationale contre le Cancer (LNCC), La Société Française de Dermatologie and Université Paris Diderot. F.K was supported by a PhD fellowship from Cancéropôle-Ile de France and from Fondation ARC pour la Recherche sur le Cancer. L.P.C was supported by a FPU fellowship from Spanish Ministry of Science. This work was supported by grant BIO2010–22324 from Plan NacionalI+D+iMICINN. We thank the core facility of the Institut Universitaire d’Hématologie for confocal microscopy analyses. The core facility is supported by grants from the Association Saint-Louis, Conseil Regional d’Ile-de-France, and the Ministère de la Recherche., Peer Reviewed, Postprint (published version)

Published
2015

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