Your search keyword '"Geneviève Huot"' showing total 10 results

1. A Hydride Transfer Complex Reprograms NAD Metabolism Preventing Senescence

Author

Gerardo Ferbeyre, Paloma Kalegari, Lian Mignacca, Frédéric Lessard, Jan Pencik, Geneviève Huot, Jordan Quenneville, Marie-Camille Rowell, Laura Hulea, Jacob Bouchard, Stéphane Lopes-Paciencia, Michael Pollak, Oro Uchenunu, Ana Fernandez-Ruiz, Katja Julissa Ponce, Etienne Gagnon, Nhung Vuong, Véronique Bourdeau, Mehdi Benfdil, Haytham M. Wahba, Ivan Topisitrovic, James G. Omichinski, Richard Moriggl, Antonio Nanci, Sebastian Igelmann, Aurélien Fouillen, David Papadopoli, and Lukas Kenner

Subjects

Senescence, chemistry.chemical_classification, Cytosol, Enzyme, Chemistry, Cancer cell, medicine, Metabolon, NAD+ kinase, Carcinogenesis, medicine.disease_cause, Cell biology, Pyruvate carboxylase

Abstract

Metabolic rewiring and redox balance play pivotal roles in cancer. Cellular senescence is a barrier for tumorigenesis circumvented in cancer cells by poorly understood mechanisms. We report a novel multi-enzymatic complex that reprograms NAD metabolism by transferring reducing equivalents from NADH to NADP +. This hydride transfer complex (HTC) is assembled by Malate Dehydrogenase-1, Malic Enzyme-1 and cytosolic Pyruvate Carboxylase. HTC enzymes are found in phase-separated bodies in the cytosol of cancer cells and can be assembled in vitro from purified proteins. They are repressed in senescent cells but induced by p53 inactivation. HTC enzymes are highly expressed in mouse and human prostate cancer models and their inactivation triggers senescence. Exogenous expression of HTC is sufficient to bypass senescence, rescue cells from complex I inhibitors and cooperate with oncogenic RAS to transform primary cells. We provide evidence for a new multi-enzymatic complex that reprograms metabolism and prevents cellular senescence.

Published

2020

2. Molecular tools that block maturation of the nuclear lamin A and decelerate cancer cell migration

Author

Alexios N. Matralis, Geneviève Huot, Hugo de Vries, Stéphane Lopes-Paciencia, Youla S. Tsantrizos, Charles Cole, Dimitrios Xanthopoulos, and Gerardo Ferbeyre

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Cell division, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Adenocarcinoma, Cleavage (embryo), Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Line, Tumor, Drug Discovery, Humans, Neoplasm Invasiveness, Molecular Biology, Mitosis, Metalloproteinase, integumentary system, Chemistry, Organic Chemistry, Membrane Proteins, Metalloendopeptidases, Cell migration, Lamin Type A, Phosphinic Acids, 3. Good health, Cell biology, 030104 developmental biology, Cancer cell, Molecular Medicine, Nuclear lamina, Peptidomimetics, 030217 neurology & neurosurgery, Lamin, Carcinoma, Pancreatic Ductal

Abstract

Lamin A contributes to the structure of nuclei in all mammalian cells and plays an important role in cell division and migration. Mature lamin A is derived from a farnesylated precursor protein, known as prelamin A, which undergoes post-translational cleavage catalyzed by the zinc metalloprotease STE24 (ZPMSTE24). Accumulation of farnesylated prelamin A in the nuclear envelope compromises cell division, impairs mitosis and induces an increased expression of inflammatory gene products. ZMPSTE24 has been proposed as a potential therapeutic target in oncology. A library of peptidomimetic compounds were synthesized and screened for their ability to induce accumulation of prelamin A in cancer cells and block cell migration in pancreatic ductal adenocarcinoma cells. The results of this study suggest that inhibitors of lamin A maturation may interfere with cell migration, the biological process required for cancer metastasis.

Published

2018

3. Senescence-associated ribosome biogenesis defects contributes to cell cycle arrest through the Rb pathway

Author

Xavier Deschênes-Simard, Marlene Oeffinger, Cornelia E. Zorca, Sebastian Igelmann, Léa Brakier-Gingras, Daniel Zenklusen, Emmanuelle Saint-Germain, Olga Moiseeva, Geneviève Huot, Neylen Del Toro, Lian Mignacca, Benjamin Le Calvé, Marinieve Montero, Marie-Camille Rowell, Frédéric Lessard, Véronique Bourdeau, Gerardo Ferbeyre, Christian Trahan, Marina Bury, and Stéphane Lopes-Paciencia

Subjects

Ribosomal Proteins, 0301 basic medicine, Senescence, Time Factors, Cell cycle checkpoint, Nucleolus, Ribosome biogenesis, Retinoblastoma Protein, 03 medical and health sciences, Ribosomal protein, Neoplasms, RNA Precursors, Humans, Phosphorylation, Cellular Senescence, Gene knockdown, Chemistry, HEK 293 cells, Cyclin-Dependent Kinase 4, RNA-Binding Proteins, Cell Cycle Checkpoints, Cell Biology, Blood Coagulation Factors, Cell biology, HEK293 Cells, 030104 developmental biology, RNA, Ribosomal, PC-3 Cells, Signal transduction, Ribosomes, Protein Binding, Signal Transduction

Abstract

Cellular senescence is a tumour suppressor programme characterized by a stable cell cycle arrest. Here we report that cellular senescence triggered by a variety of stimuli leads to diminished ribosome biogenesis and the accumulation of both rRNA precursors and ribosomal proteins. These defects were associated with reduced expression of several ribosome biogenesis factors, the knockdown of which was also sufficient to induce senescence. Genetic analysis revealed that Rb but not p53 was required for the senescence response to altered ribosome biogenesis. Mechanistically, the ribosomal protein S14 (RPS14 or uS11) accumulates in the soluble non-ribosomal fraction of senescent cells, where it binds and inhibits CDK4 (cyclin-dependent kinase 4). Overexpression of RPS14 is sufficient to inhibit Rb phosphorylation, inducing cell cycle arrest and senescence. Here we describe a mechanism for maintaining the senescent cell cycle arrest that may be relevant for cancer therapy, as well as biomarkers to identify senescent cells.

Published

2018

4. A hydride transfer complex reprograms NAD metabolism and bypasses senescence

Author

Oro Uchenunu, Gerardo Ferbeyre, James G. Omichinski, Paloma Kalegari, David Papadopoli, Antonio Nanci, Ivan Topisirovic, Jordan Quenneville, Sebastian Igelmann, Laura Hulea, Aurélien Fouillen, Lukas Kenner, Jordan Guillon, Véronique Bourdeau, Haytham M. Wahba, Jacob Bouchard, Etienne Gagnon, Richard Moriggl, Mehdi Benfdil, Jan Pencik, Marie-Camille Rowell, Katia Julissa Ponce, Frédéric Lessard, Lian Mignacca, Stéphane Lopes-Paciencia, Michael Pollak, Ana Fernandez-Ruiz, Geneviève Huot, and Nhung Vuong

Subjects

Male, Senescence, Aging, Mice, Transgenic, Biology, medicine.disease_cause, Mice, Cytosol, Malate Dehydrogenase, Mice, Inbred NOD, Cell Line, Tumor, Pyruvic Acid, medicine, Animals, Humans, Molecular Biology, Cellular Senescence, Pyruvate Carboxylase, Cell Biology, Malate dehydrogenase 1, NAD, digestive system diseases, Pyruvate carboxylase, Cell biology, Glucose, Cancer cell, NAD+ kinase, Metabolon, Carcinogenesis, Oxidation-Reduction, Hydrogen

Abstract

Metabolic rewiring and redox balance play pivotal roles in cancer. Cellular senescence is a barrier for tumorigenesis circumvented in cancer cells by poorly understood mechanisms. We report a multi-enzymatic complex that reprograms NAD metabolism by transferring reducing equivalents from NADH to NADP+. This hydride transfer complex (HTC) is assembled by malate dehydrogenase 1, malic enzyme 1, and cytosolic pyruvate carboxylase. HTC is found in phase-separated bodies in the cytosol of cancer or hypoxic cells and can be assembled in vitro with recombinant proteins. HTC is repressed in senescent cells but induced by p53 inactivation. HTC enzymes are highly expressed in mouse and human prostate cancer models, and their inactivation triggers senescence. Exogenous expression of HTC is sufficient to bypass senescence, rescue cells from complex I inhibitors, and cooperate with oncogenic RAS to transform primary cells. Altogether, we provide evidence for a new multi-enzymatic complex that reprograms metabolism and overcomes cellular senescence.

Published

2021

5. A CDK4/6-Dependent Epigenetic Mechanism Protects Cancer Cells from PML-induced Senescence

Author

Gerardo Ferbeyre, Geneviève Huot, Olga Moiseeva, Véronique Bourdeau, Frédéric Lessard, Mathieu Vernier, Mariana Acevedo, Lian Mignacca, and Université de Montréal (UdeM)

Subjects

Male, 0301 basic medicine, Senescence, Cancer Research, [SDV]Life Sciences [q-bio], Blotting, Western, Mice, Nude, Apoptosis, Promyelocytic Leukemia Protein, Real-Time Polymerase Chain Reaction, Epigenesis, Genetic, Mice, 03 medical and health sciences, 0302 clinical medicine, Cyclin-dependent kinase, Tumor Cells, Cultured, Animals, Humans, RNA, Messenger, Epigenetics, Phosphorylation, Cellular Senescence, ComputingMilieux_MISCELLANEOUS, Cell Proliferation, Regulation of gene expression, Mice, Inbred BALB C, biology, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Cell Cycle, Cyclin-Dependent Kinase 4, Prostatic Neoplasms, Cyclin-Dependent Kinase 6, DNA Methylation, Cell cycle, Xenograft Model Antitumor Assays, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, DNA methylation, biology.protein, Cyclin-dependent kinase 6

Abstract

Promyelocytic leukemia (PML) plays a tumor suppressive role by inducing cellular senescence in response to oncogenic stress. However, tumor cell lines fail to engage in complete senescence upon PML activation. In this study, we investigated the mechanisms underlying resistance to PML-induced senescence. Here, we report that activation of the cyclin-dependent kinases CDK4 and CDK6 are essential and sufficient to impair senescence induced by PML expression. Disrupting CDK function by RNA interference or pharmacological inhibition restored senescence in tumor cells and diminished their tumorigenic potential in mouse xenograft models. Complete senescence correlated with an increase in autophagy, repression of E2F target genes, and an gene expression signature of blocked DNA methylation. Accordingly, treatment of tumor cells with inhibitors of DNA methylation reversed resistance to PML-induced senescence. Further, CDK inhibition with palbociclib promoted autophagy-dependent degradation of the DNA methyltransferase DNMT1. Lastly, we found that CDK4 interacted with and phosphorylated DNMT1 in vitro, suggesting that CDK activity is required for its stabilization. Taken together, our findings highlight a potentially valuable feature of CDK4/6 inhibitors as epigenetic modulators to facilitate activation of senescence programs in tumor cells. Cancer Res; 76(11); 3252–64. ©2016 AACR.

Published

2016

6. Permanent farnesylation of lamin A mutants linked to progeria impairs its phosphorylation at serine 22 during interphase

Author

Frédéric Lessard, Olga Moiseeva, Gerardo Ferbeyre, Stéphane Lopes-Paciencia, and Geneviève Huot

Subjects

0301 basic medicine, Premature aging, Aging, congenital, hereditary, and neonatal diseases and abnormalities, senescence, Immunoblotting, Protein Prenylation, environment and public health, Serine, 03 medical and health sciences, 0302 clinical medicine, Progeria, Cyclin-dependent kinase, medicine, Humans, Immunoprecipitation, Phosphorylation, Interphase, lamin A, biology, integumentary system, nutritional and metabolic diseases, Cell Biology, medicine.disease, Progerin, Lamin Type A, Cell biology, liquid droplets, Hutchinson-Gilford progeria syndrome, 030104 developmental biology, cyclin dependent kinases, Biochemistry, Microscopy, Fluorescence, 030220 oncology & carcinogenesis, embryonic structures, Mutation, biology.protein, Mutagenesis, Site-Directed, Protein prenylation, Lamin, Research Paper

Abstract

Mutants of lamin A cause diseases including the Hutchinson-Gilford progeria syndrome (HGPS) characterized by premature aging. Lamin A undergoes a series of processing reactions, including farnesylation and proteolytic cleavage of the farnesylated C-terminal domain. The role of cleavage is unknown but mutations that affect this reaction lead to progeria. Here we show that interphase serine 22 phosphorylation of endogenous mutant lamin A (progerin) is defective in cells from HGPS patients. This defect can be mimicked by expressing progerin in human cells and prevented by inhibition of farnesylation. Furthermore, serine 22 phosphorylation of non-farnesylated progerin was enhanced by a mutation that disrupts lamin A head to tail interactions. The phosphorylation of lamin A or non-farnesylated progerin was associated to the formation of spherical intranuclear lamin A droplets that accumulate protein kinases of the CDK family capable of phosphorylating lamin A at serine 22. CDK inhibitors compromised the turnover of progerin, accelerated senescence of HGPS cells and reversed the effects of FTI on progerin levels. We discuss a model of progeria where faulty serine 22 phosphorylation compromises phase separation of lamin A polymers, leading to accumulation of functionally impaired lamin A structures.

Published

2016

7. Phosphorylation of SOCS1 Inhibits the SOCS1-p53 Tumor Suppressor Axis

Author

Geneviève Huot, Marie-Camille Rowell, Subburaj Ilangumaran, Viviane Calabrese, Mariana Acevedo, Emmanuelle Saint-Germain, Frédéric Lessard, Lian Mignacca, Gerardo Ferbeyre, Véronique Bourdeau, and Karine Moineau-Vallée

Subjects

0301 basic medicine, Cancer Research, Lymphoma, SH2 domain, src Homology Domains, 03 medical and health sciences, 0302 clinical medicine, Suppressor of Cytokine Signaling 1 Protein, Tumor Cells, Cultured, Humans, Protein Interaction Domains and Motifs, Src family kinase, Tyrosine, Phosphorylation, Cellular Senescence, Kinase, Suppressor of cytokine signaling 1, Chemistry, Cell biology, 030104 developmental biology, src-Family Kinases, Oncology, 030220 oncology & carcinogenesis, Signal transduction, Tumor Suppressor Protein p53, Tyrosine kinase, Signal Transduction

Abstract

Expression of the suppressor of cytokine signaling-1 (SOCS1) is inactivated in hematopoietic and solid cancers by promoter methylation, miRNA-mediated silencing, and mutations. Paradoxically, SOCS1 is also overexpressed in many human cancers. We report here that the ability of SOCS1 to interact with p53 and regulate cellular senescence depends on a structural motif that includes tyrosine (Y)80 in the SH2 domain of SOCS1. Mutations in this motif are found at low frequency in some human cancers, and substitution of Y80 by a phosphomimetic residue inhibits p53–SOCS1 interaction and its functional consequences, including stimulation of p53 transcriptional activity, growth arrest, and cellular senescence. Mass spectrometry confirmed SOCS1 Y80 phosphorylation in cells, and a new mAb was generated to detect its presence in tissues by IHC. A tyrosine kinase library screen identified the SRC family as Y80-SOCS1 kinases. SRC family kinase inhibitors potentiated the SOCS1–p53 pathway and reinforced SOCS1-induced senescence. Samples from human lymphomas that often overexpress SOCS1 also displayed SRC family kinase activation, constitutive phosphorylation of SOCS1 on Y80, and SOCS1 cytoplasmic localization. Collectively, these results reveal a mechanism that inactivates the SOCS1–p53 senescence pathway and suggest that inhibition of SRC family kinases as personalized treatment in patients with lymphomas may be successful. Significance: These findings show that SOCS1 phosphorylation by the SRC family inhibits its tumor-suppressive activity, indicating that patients with increased SOCS1 phosphorylation may benefit from SRC family kinase inhibitors.

Published

2018

8. CHES1/FOXN3 regulates cell proliferation by repressing PIM2 and protein biosynthesis

Author

Marie-France Gaumont-Leclerc, Laurent Doucet, Gerardo Ferbeyre, Véronique Bourdeau, Alejandro Moro, Emmanuelle Saint-Germain, Mathieu Vernier, Geneviève Huot, and Université de Montréal (UdeM)

Subjects

[SDV]Life Sciences [q-bio], Repressor, Cell Cycle Proteins, Protein Serine-Threonine Kinases, Biology, Retinoblastoma-like protein 1, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Proto-Oncogene Proteins, Protein biosynthesis, Humans, Cell Cycle Protein, Molecular Biology, Transcription factor, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Kinase, Cell growth, Forkhead Transcription Factors, Articles, Cell Biology, Fibroblasts, 3. Good health, Gene Expression Regulation, Neoplastic, Repressor Proteins, Cell Biology of Disease, Protein Biosynthesis, 030220 oncology & carcinogenesis, Cancer research, Phosphorylation

Abstract

CHES1/FOXN3 inhibits cell proliferation and protein biosynthesis in tumor cell lines but not in normal fibroblasts. CHES1 directly represses the expression of the gene coding for the protein kinase PIM2, and PIM2 or eIF4E counteracts the antiproliferative effect of CHES1. The levels of CHES1 and PIM2 are inversely correlated in several human cancers., The expression of the forkhead transcription factor checkpoint suppressor 1 (CHES1), also known as FOXN3, is reduced in many types of cancers. We show here that CHES1 decreases protein synthesis and cell proliferation in tumor cell lines but not in normal fibroblasts. Conversely, short hairpin RNA–mediated depletion of CHES1 increases tumor cell proliferation. Growth suppression depends on the CHES1 forkhead DNA-binding domain and correlates with the nuclear localization of CHES1. CHES1 represses the expression of multiple genes, including the kinases PIM2 and DYRK3, which regulate protein biosynthesis, and a number of genes in cilium biogenesis. CHES1 binds directly to the promoter of PIM2, and in cells expressing CHES1 the levels of PIM2 are reduced, as well as the phosphorylation of the PIM2 target 4EBP1. Overexpression of PIM2 or eIF4E partially reverses the antiproliferative effect of CHES1, indicating that PIM2 and protein biosynthesis are important targets of the antiproliferative effect of CHES1. In several human hematopoietic cancers, CHES1 and PIM2 expressions are inversely correlated, suggesting that repression of PIM2 by CHES1 is clinically relevant.

Published

2014

9. Metformin inhibits the senescence‐associated secretory phenotype by interfering with<scp>IKK</scp>/<scp>NF</scp>‐κ<scp>B</scp>activation

Author

Alexandra E. Cadar, Gerardo Ferbeyre, Emmanuelle St‐Germain, Sebastian Igelmann, Michael Pollak, Véronique Bourdeau, Geneviève Huot, Olga Moiseeva, and Xavier Deschênes-Simard

Subjects

Lipopolysaccharides, Male, Senescence, Aging, medicine.medical_specialty, endocrine system diseases, Gene Expression, IκB kinase, Biology, p38 Mitogen-Activated Protein Kinases, Proinflammatory cytokine, Mice, chemistry.chemical_compound, Cell Line, Tumor, Internal medicine, medicine, Animals, Humans, Hypoglycemic Agents, Phosphorylation, RNA, Small Interfering, Transcription factor, Cellular Senescence, Cell Proliferation, Inflammation, Macrophages, NF-kappa B, Transcription Factor RelA, Prostatic Neoplasms, nutritional and metabolic diseases, AMPK, NF-κB, Cell Biology, Fibroblasts, Metformin, I-kappa B Kinase, Enzyme Activation, Endocrinology, Gene Expression Regulation, chemistry, Cell culture, Culture Media, Conditioned, Cancer research, Cytokines, RNA Interference, Signal Transduction, medicine.drug

Abstract

We show that the antidiabetic drug metformin inhibits the expression of genes coding for multiple inflammatory cytokines seen during cellular senescence. Conditioned medium (CM) from senescent cells stimulates the growth of prostate cancer cells but treatment of senescent cells with metformin inhibited this effect. Bioinformatic analysis of genes downregulated by metformin suggests that the drug blocks the activity of the transcription factor NF-κB. In agreement, metformin prevented the translocation of NF-κB to the nucleus and inhibited the phosphorylation of IκB and IKKα/β, events required for activation of the NF-κB pathway. These effects were not dependent on AMPK activation or on the context of cellular senescence, as metformin inhibited the NF-κB pathway stimulated by lipopolysaccharide (LPS) in ampk null fibroblasts and in macrophages. Taken together, our results provide a novel mechanism for the antiaging and antineoplastic effects of metformin reported in animal models and in diabetic patients taking this drug.

Published

2013

10. Myc down-regulation as a mechanism to activate the Rb pathway in STAT5A-induced senescence

Author

Gerardo Ferbeyre, Frédérick A. Mallette, Geneviève Huot, and Marie-France Gaumont-Leclerc

Subjects

Senescence, Cyclin-Dependent Kinase Inhibitor p21, Proteasome Endopeptidase Complex, animal structures, Down-Regulation, Biology, Biochemistry, Models, Biological, Retinoblastoma Protein, Cell Line, Proto-Oncogene Proteins c-myc, Downregulation and upregulation, Cell Line, Tumor, STAT5 Transcription Factor, Humans, Molecular Biology, Cellular Senescence, Cell Proliferation, Cell Nucleus, Kinase, Cyclin-dependent kinase 4, Tumor Suppressor Proteins, Retinoblastoma protein, food and beverages, Cyclin-Dependent Kinase 4, Cell Biology, Fibroblasts, Cancer research, biology.protein, Signal transduction, Tumor Suppressor Protein p53, Cell aging, Signal Transduction

Abstract

Senescence is a general antiproliferative program that avoids the expansion of cells bearing oncogenic mutations. We found that constitutively active STAT5A (ca-STAT5A) can induce a p53- and Rb-dependent cellular senescence response. However, ca-STAT5A did not induce p21 and p16(INK4a), which are responsible for inhibiting cyclin-dependent protein kinases and engaging the Rb pathway during the senescence response to oncogenic ras. Intriguingly, ca-STAT5A led to a down-regulation of Myc and Myc targets, including CDK4, a negative regulator of Rb. The down-regulation of Myc was in part proteasome-dependent and correlated with its localization to promyelocytic leukemia bodies, which were found to be highly abundant during STAT5-induced senescence. Introduction of CDK4 or Myc bypassed STAT5A-induced senescence in cells in which p53 was also inactivated. These results uncover a novel mechanism to engage the Rb pathway in oncogene-induced senescence and indicate the existence of oncogene-specific pathways that regulate senescence.

Published

2007