Your search keyword '"Moreaux, Jerome"' showing total 17 results

1. Targeting the β2‐adrenergic receptor increases chemosensitivity in multiple myeloma by induction of apoptosis and modulating cancer cell metabolism.

Author

Satilmis, Hatice, Verheye, Emma, Vlummens, Philip, Oudaert, Inge, Vandewalle, Niels, Fan, Rong, Knight, Jennifer M, De Beule, Nathan, Ates, Gamze, Massie, Ann, Moreaux, Jerome, Maes, Anke, De Bruyne, Elke, Vanderkerken, Karin, Menu, Eline, Sloan, Erica K, and De Veirman, Kim

Subjects

MULTIPLE myeloma, CELL metabolism, CANCER cells, MONOCLONAL gammopathies, CARDIOVASCULAR agents, APOPTOSIS

Abstract

While multi‐drug combinations and continuous treatment have become standard for multiple myeloma, the disease remains incurable. Repurposing drugs that are currently used for other indications could provide a novel approach to improve the therapeutic efficacy of standard multiple myeloma treatments. Here, we assessed the anti‐tumor effects of cardiac drugs called β‐blockers as a single agent and in combination with commonly used anti‐myeloma therapies. Expression of the β2‐adrenergic receptor correlated with poor survival outcomes in patients with multiple myeloma. Targeting the β2‐adrenergic receptor (β2AR) using either selective or non‐selective β‐blockers reduced multiple myeloma cell viability, and induced apoptosis and autophagy. Blockade of the β2AR modulated cancer cell metabolism by reducing the mitochondrial respiration as well as the glycolytic activity. These effects were not observed by blockade of β1‐adrenergic receptors. Combining β2AR blockade with the chemotherapy drug melphalan or the proteasome inhibitor bortezomib significantly increased apoptosis in multiple myeloma cells. These data identify the therapeutic potential of β2AR‐blockers as a complementary or additive approach in multiple myeloma treatment and support the future clinical evaluation of non‐selective β‐blockers in a randomized controlled trial. © 2022 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland. [ABSTRACT FROM AUTHOR]

Published

2023

2. Comprehensive characterization of the epigenetic landscape in Multiple Myeloma.

Author

Alaterre, Elina, Ovejero, Sara, Herviou, Laurie, de Boussac, Hugues, Papadopoulos, Giorgio, Kulis, Marta, Boireau, Stéphanie, Robert, Nicolas, Requirand, Guilhem, Bruyer, Angélique, Cartron, Guillaume, Vincent, Laure, Martinez, Anne Marie, Martin-Subero, José Ignacio, Cavalli, Giacomo, and Moreaux, Jerome

Published

2022

3. Characterization of immortalized human islet stromal cells reveals a MSC-like profile with pancreatic features.

Author

Villard, Orianne, Armanet, Mathieu, Couderc, Guilhem, Bony, Claire, Moreaux, Jerome, Noël, Daniele, DeVos, John, Klein, Bernard, Veyrune, Jean-Luc, and Wojtusciszyn, Anne

Subjects

ISLANDS of Langerhans, GENE expression profiling, EXTRACELLULAR matrix, BLOOD cells, PROTEIN expression

Abstract

Background: Mesenchymal stromal cells (MSCs) represent an interesting tool to improve pancreatic islet transplantation. They have immunomodulatory properties and secrete supportive proteins. However, the functional properties of MSCs vary according to many factors such as donor characteristics, tissue origin, or isolation methods. To counteract this heterogeneity, we aimed to immortalize and characterize adherent cells derived from human pancreatic islets (hISCs), using phenotypic, transcriptomic, and functional analysis. Methods: Adherent cells derived from human islets in culture were infected with a hTERT retrovirus vector and then characterized by microarray hybridization, flow cytometry analysis, and immunofluorescence assays. Osteogenic, adipogenic, and chondrogenic differentiation as well as PBMC proliferation suppression assays were used to compare the functional abilities of hISCs and MSCs. Extracellular matrix (ECM) gene expression profile analysis was performed using the SAM (Significance Analysis of Microarrays) software, and protein expression was confirmed by western blotting. Results: hISCs kept an unlimited proliferative potential. They exhibited several properties of MSCs such as CD73, CD90, and CD105 expression and differentiation capacity. From a functional point of view, hISCs inhibited the proliferation of activated peripheral blood mononuclear cells. The transcriptomic profile of hISCs highly clusterized with bone marrow (BM)-MSCs and revealed a differential enrichment of genes involved in the organization of the ECM. Indeed, the expression and secretion profiles of ECM proteins including collagens I, IV, and VI, fibronectin, and laminins, known to be expressed in abundance around and within the islets, were different between hISCs and BM-MSCs. Conclusion: We generated a new human cell line from pancreatic islets, with MSCs properties and retaining some pancreatic specificities related to the production of ECM proteins. hISCs appear as a very promising tool in islet transplantation by their availability (as a source of inexhaustible source of cells) and ability to secrete a supportive "pancreatic" microenvironment. [ABSTRACT FROM AUTHOR]

Published

2020

4. Maternal embryonic leucine zipper kinase is a novel target for diffuse large B cell lymphoma and mantle cell lymphoma.

Author

Maes, Anke, Maes, Ken, Vlummens, Philip, De Raeve, Hendrik, Devin, Julie, Szablewski, Vanessa, De Veirman, Kim, Menu, Eline, Moreaux, Jerome, Vanderkerken, Karin, and De Bruyne, Elke

Subjects

LEUCINE zippers, MANTLE cell lymphoma, AURORA kinases, PHOSPHORYLATION, WESTERN immunoblotting, CLINICAL trials

Abstract

Diffuse large B cell lymphoma (DLBCL) and mantle cell lymphoma (MCL) are among the most aggressive B cell non-Hodgkin lymphomas. Maternal embryonic leucine zipper kinase (MELK) plays a role in cancer cell cycle progression and is associated with poor prognosis in several cancer cell types. In this study, the role of MELK in DLBCL and MCL and the therapeutic potential of MELK targeting is evaluated. MELK is highly expressed in DLBCL and MCL patient samples, correlating with a worse clinical outcome in DLBCL. Targeting MELK, using the small molecule OTSSP167, impaired cell growth and survival and induced caspase-mediated apoptosis in the lymphoma cells. Western blot analysis revealed that MELK targeting decreased the phosphorylation of FOXM1 and the protein levels of EZH2 and several mitotic regulators, such as Cdc25B, cyclin B1, Plk-1, and Aurora kinases. In addition, OTSSP167 also sensitized the lymphoma cells to the clinically relevant Bcl-2 inhibitor venetoclax by strongly reducing Mcl1 levels. Finally, OTSSP167 treatment of A20-inoculated mice resulted in a significant prolonged survival. In conclusion, targeting MELK with OTSSP167 induced strong anti-lymphoma activity both in vitro and in vivo. These findings suggest that MELK could be a potential new target in these aggressive B cell malignancies. [ABSTRACT FROM AUTHOR]

Published

2019

5. Editorial: Transcriptional control in normal and malignant B-lymphocytes.

Author

Moreaux, Jerome and Shtil, Alexander A.

Subjects

B cells, HEMATOPOIESIS

Published

2023

6. Treatment May Be Harmful: Mechanisms/Prediction/Prevention of Drug-Induced DNA Damage and Repair in Multiple Myeloma.

Author

Gourzones, Claire, Bret, Caroline, and Moreaux, Jerome

Subjects

DNA repair, DNA damage, MULTIPLE myeloma, DOUBLE-strand DNA breaks, PLASMACYTOMA, MEDICAL practice

Abstract

Multiple myeloma (MM) is a malignancy characterized by accumulation of malignant plasma cells within the bone marrow (BM). MM is considered mostly without definitive treatment because of the inability of standard of care therapies to overcome drug-resistant relapse. Genotoxic agents are used in the treatment of MM and exploit the fact that DNA double-strand breaks are highly cytotoxic for cancer cells. However, their mutagenic effects are well-established and described. According to these effects, chemotherapy could cause harmful DNA damage associated with new driver genomic abnormalities providing selective advantage, drug resistance, and higher relapse risk. Several mechanisms associated with MM cell (MMC) resistance to genotoxic agents have been described, underlining MM heterogeneity. The understanding of these mechanisms provides several therapeutic strategies to overcome drug resistance and limit mutagenic effects of treatment in MM. According to this heterogeneity, adopting precision medicine into clinical practice, with the development of biomarkers, has the potential to improve MM disease management and treatment. [ABSTRACT FROM AUTHOR]

Published

2019

7. DNMTi/HDACi combined epigenetic targeted treatment induces reprogramming of myeloma cells in the direction of normal plasma cells.

Author

Bruyer, Angelique, Maes, Ken, Herviou, Laurie, Kassambara, Alboukadel, Seckinger, Anja, Cartron, Guillaume, Rème, Thierry, Robert, Nicolas, Requirand, Guilhem, Boireau, Stéphanie, Müller-Tidow, Carsten, Veyrune, Jean-luc, Vincent, Laure, Bouhya, Salahedine, Goldschmidt, Hartmut, Vanderkerken, Karin, Hose, Dirk, Klein, Bernard, De Bruyne, Elke, and Moreaux, Jerome

Abstract

Background: Multiple myeloma (MM) is the second most common hematologic malignancy. Aberrant epigenetic modifications have been reported in MM and could be promising therapeutic targets. As response rates are overall limited but deep responses occur, it is important to identify those patients who could indeed benefit from epigenetic-targeted therapy.Methods: Since HDACi and DNMTi combination have potential therapeutic value in MM, we aimed to build a GEP-based score that could be useful to design future epigenetic-targeted combination trials. In addition, we investigated the changes in GEP upon HDACi/DNMTi treatment.Results: We report a new gene expression-based score to predict MM cell sensitivity to the combination of DNMTi/HDACi. A high Combo score in MM patients identified a group with a worse overall survival but a higher sensitivity of their MM cells to DNMTi/HDACi therapy compared to a low Combo score. In addition, treatment with DNMTi/HDACi downregulated IRF4 and MYC expression and appeared to induce a mature BMPC plasma cell gene expression profile in myeloma cell lines.Conclusion: In conclusion, we developed a score for the prediction of primary MM cell sensitivity to DNMTi/HDACi and found that this combination could be beneficial in high-risk patients by targeting proliferation and inducing maturation. [ABSTRACT FROM AUTHOR]

Published

2018

8. Identifying high-risk adult AML patients: epigenetic and genetic risk factors and their implications for therapy.

Author

Bret, Caroline, Viziteu, Elena, Kassambara, Alboukadel, and Moreaux, Jerome

Published

2016

9. Chetomin, targeting HIF-1α/p300 complex, exhibits antitumour activity in multiple myeloma.

Author

Viziteu, Elena, Grandmougin, Camille, Goldschmidt, Hartmut, Seckinger, Anja, Hose, Dirk, Klein, Bernard, and Moreaux, Jerome

Subjects

ALKALOIDS, ANTINEOPLASTIC agents, CELL lines, CELL physiology, DRUG therapy, CLINICAL drug trials, GENES, MULTIPLE myeloma, PROGNOSIS, PROTEINS, SULFUR compounds, TRANSFERASES, GENE expression profiling

Abstract

Background: Multiple myeloma (MM) is an incurable clonal plasma cell malignancy. The constitutive expression of HIF-1α in MM suggests that inhibition of HIF-1α-mediated transcription represents an interesting target in MM.Methods: As p300 is a crucial co-activator of hypoxia-inducible transcription, disrupting the complex HIF-1α/p300 to target HIF activity appears to be an attractive strategy.Results: We reported that chetomin, an inhibitor of HIF-1α/p300 interaction, exhibits antitumour activity in human myeloma cell lines and primary MM cells from patients.Conclusions: Our data suggest that chetomin may be of clinical value in MM and especially for patients characterised by a high EP300/HIF-1α expression and a poor prognosis. [ABSTRACT FROM AUTHOR]

Published

2016

10. RECQ helicases are deregulated in hematological malignancies in association with a prognostic value.

Author

Viziteu, Elena, Kassambara, Alboukadel, Pasero, Philippe, Klein, Bernard, and Moreaux, Jerome

Published

2016

11. DNA methylation score is predictive of myeloma cell sensitivity to 5-azacitidine.

Author

Moreaux, Jerome, Bruyer, Angelique, Veyrune, Jean‐Luc, Goldschmidt, Hartmut, Hose, Dirk, and Klein, Bernard

Subjects

DNA modification & restriction, CANCER pathophysiology, CANCER genetics, HEMATOLOGIC malignancies, DNA methylation, DNA methyltransferases, DECITABINE, DNA damage

Abstract

The article focuses on the role of epigenetic modifications in cancer physiopathology including haematological malignancies. Topics discussed include analysis of DNA hypomethylation during myelomagenesis in multiple myeloma, role of DNA methyltransferases in the regulation of DNA methylation, and aspects of epigenetic modifiers 5-azacytidine and decitabine which results in DNA damage induction, and DNA hypomethylation.

Published

2014

12. NPM1 is overexpressed in hyperdiploid multiple myeloma due to a gain of chromosome 5 but is not delocalized to the cytoplasm.

Author

Weinhold, Niels, Moreaux, Jerome, Raab, Marc S., Hose, Dirk, Hielscher, Thomas, Benner, Axel, Meißner, Tobias, Ehrbrecht, Edith, Brough, Michaela, Jauch, Anna, Goldschmidt, Hartmut, Klein, Bernard, and Moos, Marion

Published

2010

13. Survival and proliferation factors of normal and malignant plasma cells.

Author

Klein, Bernard, Tarte, Karin, Jourdan, Michel, Mathouk, Karene, Moreaux, Jerome, Jourdan, Eric, Legouffe, Eric, De Vos, John, and Rossi, Jean François

Abstract

Since the first identification of interleukin (IL)-6 as a myeloma cell growth factor by Dr. Kawano's and Dr. Klein's groups 14 years ago, numerous studies have emphasized its major roles in the emergence of malignant plasma cells in vivo and in the generation of normal plasma cells. Four transcription factors control B-cell differentiation into plasma cells. The B-cell transcription factor pax-5 is mainly responsible for a B-cell phenotype, and bcl-6 represses the plasma cell transcription factor blimp-1 and plasma cell differentiation. bcl-6 expression is triggered by CD40 and IL-4 activation. A lack of CD40 and IL-4 activation yields a down-regulation of bcl-6 expression, and IL-6 stimulation yields an up-regulation of blimp-1, mainly through STAT3 activation. Blimp-1 further down-regulates bcl-6 and pax-5 expression and makes plasma cell differentiation possible. IL-6 as well as IL-10 up-regulate XBP-1. XBP-1 is another transcription factor that is involved in plasma cell differentiation and whose gene expression is shut down by pax-5. The plasma cell transcription factors blimp-1 and XBP-1 are up-regulated, and the B-cell transcription factors bcl-6 and pax-5 are down-regulated, in malignant cells compared to B-cells. Apart from the recent identification of these 4 transcription factors, the factors involved in normal plasma cell generation are mostly unknown. Regarding malignant plasma cells, 3 categories of growth factors have been identified: (1) the IL-6 family cytokines, IL-10, and interferon alpha that activate the Janus kinase-signal transducer and activator of transcription (JAK/STAT) and mitogen-activated protein (MAP) kinase pathways; (2) growth factors activating the phosphatidylinositol (PI)-3 kinase/AKT and MAP kinase pathways, unlike the JAK/STAT pathway (insulin-like growth factor 1, hepatocyte growth factor, and members of the epidermal growth factor family able to bind syndecan-1 proteoglycan); and (3) B-cell-activating factor (BAFF) or proliferation-inducing ligand (APRIL) that activate the nuclear factor KB and PI-3 kinase/AKT pathways. BAFF and APRIL bind to BAFF receptor and TACI and are major B-cell survival factors. Recent data indicate that these various growth factors may cooperate to provide optimum signaling because they are localized together and with cytoplasmic transduction elements in caveolinlinked membrane caveolae. The identification of these myeloma cell growth factors and of the associated transduction pathways should provide novel therapeutic targets in multiple myeloma. [ABSTRACT FROM AUTHOR]

Published

2003

14. Clinical Correlations of Polycomb Repressive Complex 2 in Different Tumor Types.

Author

Erokhin, Maksim, Chetverina, Olga, Győrffy, Balázs, Tatarskiy, Victor V., Mogila, Vladic, Shtil, Alexander A., Roninson, Igor B., Moreaux, Jerome, Georgiev, Pavel, Cavalli, Giacomo, and Chetverina, Darya

Subjects

TUMOR classification, GENETIC mutation, LIVER tumors, GLIOMAS, REGRESSION analysis, GENE expression, GENOMICS, GENE expression profiling, KIDNEY tumors, SURVIVAL analysis (Biometry), KAPLAN-Meier estimator, DESCRIPTIVE statistics, TRANSCRIPTION factors, GENE amplification, CRISPRS, CELL lines, STATISTICAL correlation, PROSTATE tumors, PROPORTIONAL hazards models

Abstract

Simple Summary: PRC2 (Polycomb repressive complex 2) is a catalytic multi-subunit complex involved in transcriptional repression through the methylation of lysine 27 at histone 3 (H3K27me1/2/3). Dysregulation of PRC2 has been linked to tumor development and progression. Here, we performed a comprehensive analysis of data in the genomic and transcriptomic (cBioPortal, KMplot) database portals of clinical tumor samples and evaluated clinical correlations of EZH2, SUZ12, and EED. Next, we developed an original Python application enabling the identification of genes cooperating with PRC2 in oncogenic processes for the analysis of the DepMap CRISPR knockout database. Our study identified cancer types that are most likely to be responsive to PRC2 inhibitors. By analyzing co-dependencies with other genes, this analysis also provides indications of prognostic biomarkers and new therapeutic regimens. PRC2 (Polycomb repressive complex 2) is an evolutionarily conserved protein complex required to maintain transcriptional repression. The core PRC2 complex includes EZH2, SUZ12, and EED proteins and methylates histone H3K27. PRC2 is known to contribute to carcinogenesis and several small molecule inhibitors targeting PRC2 have been developed. The present study aimed to identify the cancer types in which PRC2 targeting drugs could be beneficial. We queried genomic and transcriptomic (cBioPortal, KMplot) database portals of clinical tumor samples to evaluate clinical correlations of PRC2 subunit genes. EZH2, SUZ12, and EED gene amplification was most frequently found in prostate cancer, whereas lymphoid malignancies (DLBCL) frequently showed EZH2 mutations. In both cases, PRC2 alterations were associated with poor prognosis. Moreover, higher expression of PRC2 subunits was correlated with poor survival in renal and liver cancers as well as gliomas. Finally, we generated a Python application to analyze the correlation of EZH2/SUZ12/EED gene knockouts by CRISPR with the alterations detected in the cancer cell lines using DepMap data. As a result, we were able to identify mutations that correlated significantly with tumor cell sensitivity to PRC2 knockout, including SWI/SNF, COMPASS/COMPASS-like subunits and BCL2, warranting the investigation of these genes as potential markers of sensitivity to PRC2-targeting drugs. [ABSTRACT FROM AUTHOR]

Published

2021

15. Role of Polycomb Complexes in Normal and Malignant Plasma Cells.

Author

Varlet, Emmanuel, Ovejero, Sara, Martinez, Anne-Marie, Cavalli, Giacomo, and Moreaux, Jerome

Subjects

PLASMA cells, PLASMA cell diseases, PLASMACYTOMA, BONE marrow, CELL differentiation, MULTIPLE myeloma

Abstract

Plasma cells (PC) are the main effectors of adaptive immunity, responsible for producing antibodies to defend the body against pathogens. They are the result of a complex highly regulated cell differentiation process, taking place in several anatomical locations and involving unique genetic events. Pathologically, PC can undergo tumorigenesis and cause a group of diseases known as plasma cell dyscrasias, including multiple myeloma (MM). MM is a severe disease with poor prognosis that is characterized by the accumulation of malignant PC within the bone marrow, as well as high clinical and molecular heterogeneity. MM patients frequently develop resistance to treatment, leading to relapse. Polycomb group (PcG) proteins are epigenetic regulators involved in cell fate and carcinogenesis. The emerging roles of PcG in PC differentiation and myelomagenesis position them as potential therapeutic targets in MM. Here, we focus on the roles of PcG proteins in normal and malignant plasma cells, as well as their therapeutic implications. [ABSTRACT FROM AUTHOR]

Published

2020

16. Correction to: Characterization of immortalized human islet stromal cells reveals a MSC-like profile with pancreatic features.

Author

Villard, Orianne, Armanet, Mathieu, Couderc, Guilhem, Bony, Claire, Moreaux, Jerome, Noël, Daniele, De Vos, John, Klein, Bernard, Veyrune, Jean-Luc, and Wojtusciszyn, Anne

Subjects

ISLANDS of Langerhans, STROMAL cells

Abstract

An amendment to this paper has been published and can be accessed via the original article. [ABSTRACT FROM AUTHOR]

Published

2020

17. PRC2 targeting is a therapeutic strategy for EZ score defined high-risk multiple myeloma patients and overcome resistance to IMiDs.

Author

Herviou, Laurie, Kassambara, Alboukadel, Boireau, Stéphanie, Robert, Nicolas, Requirand, Guilhem, Müller-Tidow, Carsten, Vincent, Laure, Seckinger, Anja, Goldschmidt, Hartmut, Cartron, Guillaume, Hose, Dirk, Cavalli, Giacomo, and Moreaux, Jerome

Subjects

POLYCOMB group proteins, MULTIPLE myeloma, PLASMA cell diseases

Abstract

Background: Multiple myeloma (MM) is a malignant plasma cell disease with a poor survival, characterized by the accumulation of myeloma cells (MMCs) within the bone marrow. Epigenetic modifications in MM are associated not only with cancer development and progression, but also with drug resistance. Methods: We identified a significant upregulation of the polycomb repressive complex 2 (PRC2) core genes in MM cells in association with proliferation. We used EPZ-6438, a specific small molecule inhibitor of EZH2 methyltransferase activity, to evaluate its effects on MM cells phenotype and gene expression prolile. Results: PRC2 targeting results in growth inhibition due to cell cycle arrest and apoptosis together with polycomb, DNA methylation, TP53, and RB1 target genes induction. Resistance to EZH2 inhibitor is mediated by DNA methylation of PRC2 target genes. We also demonstrate a synergistic effect of EPZ-6438 and lenalidomide, a conventional drug used for MM treatment, activating B cell transcription factors and tumor suppressor gene expression in concert with MYC repression. We establish a gene expression-based EZ score allowing to identify poor prognosis patients that could benefit from EZH2 inhibitor treatment. Conclusions: These data suggest that PRC2 targeting in association with IMiDs could have a therapeutic interest in MM patients characterized by high EZ score values, reactivating B cell transcription factors, and tumor suppressor genes. [ABSTRACT FROM AUTHOR]

Published

2018