Your search keyword '"Alessandra Mauri-Crouzet"' showing total 7 results

1. CHCHD10S59L/+ mouse model: Behavioral and neuropathological features of frontotemporal dementia

Author

Emmanuelle C. Genin, Pauline Pozzo di Borgo, Thomas Lorivel, Sandrine Hugues, Mélissa Farinelli, Alessandra Mauri-Crouzet, Françoise Lespinasse, Lucas Godin, Véronique Paquis-Flucklinger, and Agnès Petit-Paitel

Subjects

CHCHD10, Mitochondrion, Frontotemporal dementia, Amyotrophic lateral sclerosis, Mouse model, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

CHCHD10-related disease causes a spectrum of clinical presentations including mitochondrial myopathy, cardiomyopathy, amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). We generated a knock-in mouse model bearing the p.Ser59Leu (S59L) CHCHD10 variant. Chchd10S59L/+ mice have been shown to phenotypically replicate the disorders observed in patients: myopathy with mtDNA instability, cardiomyopathy and typical ALS features (protein aggregation, neuromuscular junction degeneration and spinal motor neuron loss). Here, we conducted a comprehensive behavioral, electrophysiological and neuropathological assessment of Chchd10S59L/+ mice. These animals show impaired learning and memory capacities with reduced long-term potentiation (LTP) measured at the Perforant Pathway-Dentate Gyrus (PP-DG) synapses. In the hippocampus of Chchd10S59L/+ mice, neuropathological studies show the involvement of protein aggregates, activation of the integrated stress response (ISR) and neuroinflammation in the degenerative process. These findings contribute to decipher mechanisms associated with CHCHD10 variants linking mitochondrial dysfunction and neuronal death. They also validate the Chchd10S59L/+ mice as a relevant model for FTD, which can be used for preclinical studies to test new therapeutic strategies for this devastating disease.

Published

2024

2. Loss of MICOS complex integrity and mitochondrial damage, but not TDP-43 mitochondrial localisation, are likely associated with severity of CHCHD10-related diseases

Author

Emmanuelle C. Genin, Sylvie Bannwarth, Françoise Lespinasse, Bernardo Ortega-Vila, Konstantina Fragaki, Kie Itoh, Elodie Villa, Sandra Lacas-Gervais, Manu Jokela, Mari Auranen, Emil Ylikallio, Alessandra Mauri-Crouzet, Henna Tyynismaa, Anna Vihola, Gaelle Augé, Charlotte Cochaud, Hiromi Sesaki, Jean-Ehrland Ricci, Bjarne Udd, Cristofol Vives-Bauza, and Véronique Paquis-Flucklinger

Subjects

CHCHD10, SMAJ, FTD-ALS, Mitochondria, TDP-43, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Following the involvement of CHCHD10 in FrontoTemporal-Dementia-Amyotrophic Lateral Sclerosis (FTD-ALS) clinical spectrum, a founder mutation (p.Gly66Val) in the same gene was identified in Finnish families with late-onset spinal motor neuronopathy (SMAJ). SMAJ is a slowly progressive form of spinal muscular atrophy with a life expectancy within normal range. In order to understand why the p.Ser59Leu mutation, responsible for severe FTD-ALS, and the p.Gly66Val mutation could lead to different levels of severity, we compared their effects in patient cells. Unlike affected individuals bearing the p.Ser59Leu mutation, patients presenting with SMAJ phenotype have neither mitochondrial myopathy nor mtDNA instability. The expression of CHCHD10S59L mutant allele leads to disassembly of mitochondrial contact site and cristae organizing system (MICOS) with mitochondrial dysfunction and loss of cristae in patient fibroblasts. We also show that G66V fibroblasts do not display the loss of MICOS complex integrity and mitochondrial damage found in S59L cells. However, S59L and G66V fibroblasts show comparable accumulation of phosphorylated mitochondrial TDP-43 suggesting that the severity of phenotype and mitochondrial damage do not depend on mitochondrial TDP-43 localization. The expression of the CHCHD10G66V allele is responsible for mitochondrial network fragmentation and decreased sensitivity towards apoptotic stimuli, but with a less severe effect than that found in cells expressing the CHCHD10S59L allele.Taken together, our data show that cellular phenotypes associated with p.Ser59Leu and p.Gly66Val mutations in CHCHD10 are different; loss of MICOS complex integrity and mitochondrial dysfunction, but not TDP-43 mitochondrial localization, being likely essential to develop a severe motor neuron disease.

Published

2018

3. CHCHD10 and SLP2 control the stability of the PHB complex: a key factor for motor neuron viability

Author

Emmanuelle C Genin, Sylvie Bannwarth, Baptiste Ropert, Françoise Lespinasse, Alessandra Mauri-Crouzet, Gaelle Augé, Konstantina Fragaki, Charlotte Cochaud, Erminia Donnarumma, Sandra Lacas-Gervais, Timothy Wai, Véronique Paquis-Flucklinger, Institut de Recherche sur le Cancer et le Vieillissement (IRCAN), Université Nice Sophia Antipolis (1965 - 2019) (UNS), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Côte d'Azur (UCA), Biologie mitochondriale – Mitochondrial biology, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Centre Commun de Microscopie Appliquée (CCMA), Université de Nice Sophia-Antipolis (UNSA), This work was made possible by grants to V.P.-F. from the ANR (Agence Nationale de la Recherche) ANR-16-CE16-0024-01 and from the FRM (Fondation pour la Recherche Médicale) FRM: MND202004011475., We acknowledge Thibault Léger and the Proteomics facility of the Institut Jacques Monod, University of Paris Cité for mass spectrometry analysis. We also thank Christelle Boscagli for technical help. We gratefully acknowledge the IRCAN’s Molecular and Cellular Core Imaging (PICMI) facility, supported financially by FEDER, Conseil régional Provence Alpes-Côte d’Azur, Conseil Départemental 06, Cancéropôle PACA, Gis Ibisa and Inserm, the IRCAN’s Animal core facility, supported by FEDER, Région Provence Alpes-Côte d’Azur, Conseil Départemental 06 and Inserm, the IRCAN’s Histology core facility, supported by Région Provence Alpes-Côte d’Azur, Cancéropôle PACA and Université Côte d’Azur and, the University’s CCMA Electron Microscopy facility supported by Université Côte d’Azur, Région Provence Alpes-Côte d’Azur, Conseil Départemental 06 and Gis Ibisa, ANR-16-CE16-0024,MicroGol,Implication des fonctions sécrétoires de l'appareil de Golgi dans le développement des microcéphalies postnatales avec déficit intellectuel(2016), Lemesle, Marie, and Implication des fonctions sécrétoires de l'appareil de Golgi dans le développement des microcéphalies postnatales avec déficit intellectuel - - MicroGol2016 - ANR-16-CE16-0024 - AAPG2016 - VALID

Subjects

Motor Neurons, PHB = prohibitin, Amyotrophic Lateral Sclerosis, Membrane Proteins, PLA = proximity ligation assay, MICOS = mitochondrial contact site and cristae organizing system, MESH: Amyotrophic Lateral Sclerosis* / genetics Amyotrophic Lateral Sclerosis* / metabolism Animals Frontotemporal Dementia* / genetics Humans Membrane Proteins* / genetics Membrane Proteins* / metabolism Mice Mitochondria / metabolism Mitochondrial Proteins* / genetics Mitochondrial Proteins* / metabolism Motor Neurons / metabolism Prohibitins Transcription Factors / genetics, IMM = inner mitochondrial membrane, Mitochondria, Mitochondrial Proteins, Mice, ALS = amyotrophic lateral sclerosis, [SDV.SPEE] Life Sciences [q-bio]/Santé publique et épidémiologie, Frontotemporal Dementia, Prohibitins, motor neuron disease, mitochondrion, Animals, Humans, FTD = frontotemporal dementia, [SDV.SPEE]Life Sciences [q-bio]/Santé publique et épidémiologie, Neurology (clinical), RC = respiratory chain, MN = motor neuron, Transcription Factors

Abstract

CHCHD10 is an amyotrophic lateral sclerosis/frontotemporal dementia gene that encodes a mitochondrial protein whose precise function is unclear. Here we show that Coiled-Coil-Helix-Coiled-Coil-Helix Domain Containing protein 10 interacts with the Stomatin-Like Protein 2 and participates in the stability of the prohibitin complex in the inner mitochondrial membrane. By using patient fibroblasts and mouse models expressing the same CHCHD10 variant (p.Ser59Leu), we show that Stomatin-Like Protein 2 forms aggregates with prohibitins, found in vivo in the hippocampus and as aggresome-like inclusions in spinal motor neurons of Chchd10S59L/+ mice. Affected cells and tissues display instability of the prohibitin complex, which participates at least in part in the activation of the OMA1 cascade with OPA1 processing leading to mitochondrial fragmentation, abnormal mitochondrial cristae morphogenesis and neuronal death found in spinal cord and the hippocampus of Chchd10S59L/+ animals. Destabilization of the prohibitin complex leads to the instability of the mitochondrial contact site and cristae organizing the system complex, probably by the disruption of OPA1–mitofilin interaction. Thus, Stomatin-Like Protein 2/prohibitin aggregates and destabilization of the prohibitin complex are critical in the sequence of events leading to motor neuron death in CHCHD10S59L-related disease.

Published

2021

4. SLP2/prohibitins aggregates and instability of the PHB complex are key elements in CHCHD10S59L-related disease

Author

Paquis-Flucklinger, Gaëlle Augé, Alessandra Mauri-Crouzet, Charlotte Cochaud, Ropert B, Sylvie Bannwarth, Françoise Lespinasse, Konstantina Fragaki, Sandra Lacas-Gervais, and Emmanuelle Génin

Subjects

MICOS complex, medicine.diagnostic_test, Chemistry, Apoptosis, Proteolysis, Mitophagy, medicine, PINK1, Mitochondrion, Prohibitin, Inner mitochondrial membrane, Cell biology

Abstract

CHCHD10 is an ALS/FTD gene, also involved in a large clinical spectrum, that encodes a protein whose precise function within mitochondria is unclear. Here we show that CHCHD10 interacts with the Stomatin-Like Protein 2 (SLP2) to control the stability of the Prohibitin (PHB) complex in the inner mitochondrial membrane. In affected tissues, SLP2 forms aggregates with prohibitins and the instability of the PHB complex results in activation of OMA1 and accelerated OPA1 proteolysis leading to mitochondrial fragmentation, loss of mitochondrial cristae and apoptosis. Abnormal cristae morphogenesis depends on both the PHB complex destabilization leading to MICOS complex instability, via disruption of OPA1/Mitofilin interaction, and the activation of PINK1-mediated pathways. We also show that the increase of mitophagy found in both heart and hippocampus of Chchd10S59L/+ mito-QC mice is PINK1/Parkin-dependent. Thus, SLP2/PHBs aggregates and destabilization of the PHB complex with PINK1 activation are critical in the sequence of events leading to CHCHD10S59L-related disease.

Published

2021

5. Mitochondrial defect in muscle precedes neuromuscular junction degeneration and motor neuron death in CHCHD10S59L/+ mouse

Author

Blandine Madji Hounoum, Françoise Lespinasse, Alessandra Mauri-Crouzet, Delphine Bohl, Fanny Mochel, Emmanuelle Génin, Jean-Ehrland Ricci, Aude Chiot, Véronique Paquis-Flucklinger, Charlotte Cochaud, Julien Neveu, Cynthia Lefebvre-Omar, Sandra Lacas-Gervais, Konstantina Fragaki, Stéphanie Bigou, Gaëlle Augé, Christian S. Lobsiger, Séverine Boillée, Sylvie Bannwarth, Baptiste Ropert, CCMA - Centre Commun de Microscopie Appliquée, and Université Nice Côte D'Azur

Subjects

0301 basic medicine, [SDV]Life Sciences [q-bio], Motor neuron, Biology, Mitochondrion, Neurotransmission, medicine.disease, Spinal cord, Neuromuscular junction, 3. Good health, Pathology and Forensic Medicine, Cell biology, 03 medical and health sciences, Cellular and Molecular Neuroscience, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Mitochondrial myopathy, Mitophagy, medicine, Neurology (clinical), Amyotrophic lateral sclerosis, 030217 neurology & neurosurgery, ComputingMilieux_MISCELLANEOUS

Abstract

Recently, we provided genetic basis showing that mitochondrial dysfunction can trigger motor neuron degeneration, through identification of CHCHD10 encoding a mitochondrial protein. We reported patients, carrying the p.Ser59Leu heterozygous mutation in CHCHD10, from a large family with a mitochondrial myopathy associated with motor neuron disease (MND). Rapidly, our group and others reported CHCHD10 mutations in amyotrophic lateral sclerosis (ALS), frontotemporal dementia-ALS and other neurodegenerative diseases. Here, we generated knock-in (KI) mice, carrying the p.Ser59Leu mutation, that mimic the mitochondrial myopathy with mtDNA instability displayed by the patients from our original family. Before 14 months of age, all KI mice developed a fatal mitochondrial cardiomyopathy associated with enhanced mitophagy. CHCHD10S59L/+ mice also displayed neuromuscular junction (NMJ) and motor neuron degeneration with hyper-fragmentation of the motor end plate and moderate but significant motor neuron loss in lumbar spinal cord at the end stage of the disease. At this stage, we observed TDP-43 cytoplasmic aggregates in spinal neurons. We also showed that motor neurons differentiated from human iPSC carrying the p.Ser59Leu mutation were much more sensitive to Staurosporine or glutamate-induced caspase activation than control cells. These data confirm that mitochondrial deficiency associated with CHCHD10 mutations can be at the origin of MND. CHCHD10 is highly expressed in the NMJ post-synaptic part. Importantly, the fragmentation of the motor end plate was associated with abnormal CHCHD10 expression that was also observed closed to NMJs which were morphologically normal. Furthermore, we found OXPHOS deficiency in muscle of CHCHD10S59L/+ mice at 3 months of age in the absence of neuron loss in spinal cord. Our data show that the pathological effects of the p.Ser59Leu mutation target muscle prior to NMJ and motor neurons. They likely lead to OXPHOS deficiency, loss of cristae junctions and destabilization of internal membrane structure within mitochondria at motor end plate of NMJ, impairing neurotransmission. These data are in favor with a key role for muscle in MND associated with CHCHD10 mutations.

Published

2019

6. Mitochondrial defect in muscle precedes neuromuscular junction degeneration and motor neuron death in CHCHD10

Author

Emmanuelle C, Genin, Blandine, Madji Hounoum, Sylvie, Bannwarth, Konstantina, Fragaki, Sandra, Lacas-Gervais, Alessandra, Mauri-Crouzet, Françoise, Lespinasse, Julien, Neveu, Baptiste, Ropert, Gaelle, Augé, Charlotte, Cochaud, Cynthia, Lefebvre-Omar, Stéphanie, Bigou, Aude, Chiot, Fanny, Mochel, Séverine, Boillée, Christian S, Lobsiger, Delphine, Bohl, Jean-Ehrland, Ricci, and Véronique, Paquis-Flucklinger

Subjects

DNA-Binding Proteins, Mitochondrial Proteins, Motor Neurons, Phenotype, Cell Death, Frontotemporal Dementia, Amyotrophic Lateral Sclerosis, Nerve Degeneration, Neuromuscular Junction, Animals, Mice, Transgenic, Mitochondria

Abstract

Recently, we provided genetic basis showing that mitochondrial dysfunction can trigger motor neuron degeneration, through identification of CHCHD10 encoding a mitochondrial protein. We reported patients, carrying the p.Ser59Leu heterozygous mutation in CHCHD10, from a large family with a mitochondrial myopathy associated with motor neuron disease (MND). Rapidly, our group and others reported CHCHD10 mutations in amyotrophic lateral sclerosis (ALS), frontotemporal dementia-ALS and other neurodegenerative diseases. Here, we generated knock-in (KI) mice, carrying the p.Ser59Leu mutation, that mimic the mitochondrial myopathy with mtDNA instability displayed by the patients from our original family. Before 14 months of age, all KI mice developed a fatal mitochondrial cardiomyopathy associated with enhanced mitophagy. CHCHD10

Published

2018

7. Loss of MICOS complex integrity and mitochondrial damage, but not TDP-43 mitochondrial localisation, are likely associated with severity of CHCHD10-related diseases

Author

Emil Ylikallio, Mari Auranen, Charlotte Cochaud, Jean-Ehrland Ricci, Alessandra Mauri-Crouzet, Henna Tyynismaa, Anna Vihola, Bjarne Udd, Véronique Paquis-Flucklinger, Cristofol Vives-Bauza, Bernardo Ortega-Vila, Gaëlle Augé, Emmanuelle Génin, Manu Jokela, Konstantina Fragaki, Françoise Lespinasse, Sandra Lacas-Gervais, Hiromi Sesaki, Sylvie Bannwarth, Kie Itoh, Elodie Villa, CCMA - Centre Commun de Microscopie Appliquée, Université Nice Côte D'Azur, Research Programs Unit, Clinicum, Department of Neurosciences, Neurologian yksikkö, University of Helsinki, Research Programme for Molecular Neurology, Centre of Excellence in Stem Cell Metabolism, Medicum, Doctoral Programme Brain & Mind, Henna Tyynismaa / Principal Investigator, Department of Medical and Clinical Genetics, Doctoral Programme in Integrative Life Science, and HUS Neurocenter

Subjects

Male, 0301 basic medicine, Mitochondrial Diseases, TDP-43, [SDV]Life Sciences [q-bio], Mitochondrion, medicine.disease_cause, Severity of Illness Index, AMYOTROPHIC-LATERAL-SCLEROSIS, 3124 Neurology and psychiatry, 0302 clinical medicine, Mitochondrial myopathy, MOTOR-NEURON DISEASE, ComputingMilieux_MISCELLANEOUS, Mutation, MICOS complex, Neurodegeneration, NEURODEGENERATION, Middle Aged, Mitochondria, Cell biology, DNA-Binding Proteins, Neurology, Frontotemporal Dementia, Female, Adult, Mitochondrial DNA, Saccharomyces cerevisiae Proteins, Biology, PATIENT, Article, lcsh:RC321-571, Mitochondrial Proteins, 03 medical and health sciences, medicine, Humans, Allele, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, FRONTOTEMPORAL LOBAR DEGENERATION, HEXANUCLEOTIDE REPEAT, Amyotrophic Lateral Sclerosis, 3112 Neurosciences, Membrane Proteins, Spinal muscular atrophy, medicine.disease, ta3124, INDIVIDUALS, CHCHD10 MUTATIONS, HEK293 Cells, CHCHD10, 030104 developmental biology, SMAJ, CELLS, FTD-ALS, ALS, 030217 neurology & neurosurgery, HeLa Cells

Abstract

Following the involvement of CHCHD10 in FrontoTemporal-Dementia-Amyotrophic Lateral Sclerosis (FTD-ALS) clinical spectrum, a founder mutation (p.Gly66Val) in the same gene was identified in Finnish families with late onset spinal motor neuronopathy (SMAJ). SMAJ is a slowly progressive form of spinal muscular atrophy with a life expectancy within normal range. In order to understand why the p.Ser59Leu mutation, responsible for severe FTD-ALS, and the p.Gly66Val mutation could lead to different levels of severity, we compared their effects in patient cells. Unlike affected individuals bearing the p.Ser59Leu mutation, patients presenting with SMAJ phenotype have neither mitochondrial myopathy nor mtDNA instability. The expression of CHCHD10(S59L) mutant allele leads to disassembly of mitochondrial contact site and cristae organizing system (MICOS) with mitochondria] dysfunction and loss of cristae in patient fibroblasts. We also show that G66V fibroblasts do not display the loss of MICOS complex integrity and mitochondrial damage found in S59L cells. However, S59L and G66V fibroblasts show comparable accumulation of phosphorylated mitochondrial TDP-43 suggesting that the severity of phenotype and mitochondrial damage do not depend on mitochondrial TDP-43 localization. The expression of the CHCHD10(G66V) allele is responsible for mitochondrial network fragmentation and decreased sensitivity towards apoptotic stimuli, but with a less severe effect than that found in cells expressing the CHCHD10(S59L) allele. Taken together, our data show that cellular phenotypes associated with p.Ser59Leu and p.Gly66Val mutations in CHCHD10 are different; loss of MICOS complex integrity and mitochondrial dysfunction, but not TDP-43 mitochondrial localization, being likely essential to develop a severe motor neuron disease.

Published

2018