Your search keyword '"Maltecca, F."' showing total 35 results

1. A novel AFG3L2 mutation close to AAA domain leads to aberrant OMA1 and OPA1 processing in a family with optic atrophy

Author

Baderna, V, Schultz, J, Kearns, LS, Fahey, M, Thompson, BA, Ruddle, JB, Huq, A, Maltecca, F, Baderna, V, Schultz, J, Kearns, LS, Fahey, M, Thompson, BA, Ruddle, JB, Huq, A, and Maltecca, F

Abstract

Autosomal dominant optic atrophy (ADOA) is a neuro-ophthalmic condition characterized by bilateral degeneration of the optic nerves. Although heterozygous mutations in OPA1 represent the most common genetic cause of ADOA, a significant number of cases remain undiagnosed.Here, we describe a family with a strong ADOA history with most family members spanning three generation having childhood onset of visual symptoms. The proband, in addition to optic atrophy, had neurological symptoms consistent with relapsing remitting multiple sclerosis. Clinical exome analysis detected a novel mutation in the AFG3L2 gene (NM_006796.2:c.1010G > A; p.G337E), which segregated with optic atrophy in family members. AFG3L2 is a metalloprotease of the AAA subfamily which exerts quality control in the inner mitochondrial membrane. Interestingly, the identified mutation localizes close to the AAA domain of AFG3L2, while those localized in the proteolytic domain cause dominant spinocerebellar ataxia type 28 (SCA28) or recessive spastic ataxia with epilepsy (SPAX5). Functional studies in patient fibroblasts demonstrate that the p.G337E AFG3L2 mutation strongly destabilizes the long isoforms of OPA1 via OMA hyper-activation and leads to mitochondrial fragmentation, thus explaining the family phenotype. This study widens the clinical spectrum of neurodegenerative diseases caused by AFG3L2 mutations, which shall be considered as genetic cause of ADOA.

Published

2020

2. Dementia, ataxia, extrapyramidal features, and epilepsy: phenotype spectrum in two Italian families with spinocerebellar ataxia type 17

Author

De Michele, G., Maltecca, F., Carella, M., Volpe, G., Orio, M., De Falco, A., Gombia, S., Servadio, A., Casari, G., Filla, A., and Bruni, A.

Published

2003

3. INTERGENERATIONAL INSTABILITY AND MARKED ANTICIPATION IN SCA-17

Author

MALTECCA F, FILLA, ALESSANDRO, CASTALDO I, COPPOLA G, CARELLA M, BRUNI A, COCOZZA, SERGIO, CASARI G, SERVADIO A, DE MICHELE, GIUSEPPE, FRAGASSI, NINA ANTONETTA, Maltecca, F, Filla, Alessandro, Castaldo, I, Coppola, G, Fragassi, NINA ANTONETTA, Carella, M, Bruni, A, Cocozza, Sergio, Casari, G, Servadio, A, and DE MICHELE, Giuseppe

Published

2003

4. Clinical, neuropathological and linkage study of a kindred with autosomal dominant dementia, cerebellar and extrapyramidal features

Author

Bruni AC, De Michele G, Filla A, Carella M, D'Adamo P, Maltecca F, Servadio A, El Hachimi KH, Duyckaerts C, Foncin JF, CASARI , GIORGIO NEVIO, Bruni, Ac, De Michele, G, Filla, A, Carella, M, D'Adamo, P, Maltecca, F, Servadio, A, Casari, GIORGIO NEVIO, El Hachimi, Kh, Duyckaerts, C, and Foncin, Jf

Published

2002

5. Genome-wide expression analysis identified defects in cell growth, proliferation and viability in SCA28 lymphoblastoid cell lines

Author

Mancini, Cecilia, Roncaglia, P, Brussino, Alessandro, Stevanin, G, LO BUONO, Nicola, Krmac, H, Maltecca, F, Gazzano, Elena, Bartoletti Stella, A., Calvaruso, M. A., Iommarini, L., Cagnoli, Claudia, Forlani, S, Le Ber, I, Durr, A, Brice, A, Ghigo, Dario Antonio, Casari, G, Porcelli, Am, Funaro, Ada, Gasparre, G, Gustincich, S, and Brusco, Alfredo

Published

2013

6. A Genome-wide Expression profiling to unravel effect of missense mutations in SCA28 patients

Author

Mancini, Cecilia, Roncaglia, P, LO BUONO, Nicola, Brussino, Alessandro, Cagnoli, Claudia, Maltecca, F, Krmac, H, Limongi, T, Stevanin, G, Forlani, S, Casari, G, Funaro, Ada, Durr, A, Migone, Nicola, Gustincich, S, and Brusco, Alfredo

Subjects

SCA28, genome wide expression, ataxia, microarray analysis

Published

2011

7. Respiratory dysfunction by AFG3L2 deficiency causes decreased mitochondrial calcium uptake via organellar network fragmentation

Author

Maltecca, F., primary, De Stefani, D., additional, Cassina, L., additional, Consolato, F., additional, Wasilewski, M., additional, Scorrano, L., additional, Rizzuto, R., additional, and Casari, G., additional

Published

2012

8. Intergenerational instability and marked anticipation in SCA-17

Author

Maltecca, F., primary, Filla, A., additional, Castaldo, I., additional, Coppola, G., additional, Fragassi, N.A., additional, Carella, M., additional, Bruni, A., additional, Cocozza, S., additional, Casari, G., additional, Servadio, A., additional, and De Michele, G., additional

Published

2003

9. Upregulation of Peroxiredoxin 3 Protects Afg3l2-KO Cortical Neurons In Vitro from Oxidative Stress: A Paradigm for Neuronal Cell Survival under Neurodegenerative Conditions

Author

Franca Codazzi, Barbara Bettegazzi, Fabio Grohovaz, Francesca Maltecca, Ilaria Pelizzoni, Lisa Michelle Restelli, Daniele Zacchetti, Giorgio Casari, Floramarida Salerno Scarzella, Bettegazzi, B., Pelizzoni, I., Scarzella, F. S., Restelli, L. M., Zacchetti, D., Maltecca, F., Casari, G., Grohovaz, F., and Codazzi, F.

Subjects

Aging, Antioxidant, biology, Article Subject, Chemistry, lcsh:Cytology, medicine.medical_treatment, Cell Biology, General Medicine, Glutathione, Mitochondrion, medicine.disease_cause, Biochemistry, Neuroprotection, Cell biology, Superoxide dismutase, chemistry.chemical_compound, Downregulation and upregulation, medicine, biology.protein, lcsh:QH573-671, Peroxiredoxin, Oxidative stress

Abstract

Several neurodegenerative disorders exhibit selective vulnerability, with subsets of neurons more affected than others, possibly because of the high expression of an altered gene or the presence of particular features that make them more susceptible to insults. On the other hand, resilient neurons may display the ability to develop antioxidant defenses, particularly in diseases of mitochondrial origin, where oxidative stress might contribute to the neurodegenerative process. In this work, we investigated the oxidative stress response of embryonic fibroblasts and cortical neurons obtained from Afg3l2-KO mice. AFG3L2 encodes a subunit of a protease complex that is expressed in mitochondria and acts as both quality control and regulatory enzyme affecting respiration and mitochondrial dynamics. When cells were subjected to an acute oxidative stress protocol, the survival of AFG3L2-KO MEFs was not significantly influenced and was comparable to that of WT; however, the basal level of the antioxidant molecule glutathione was higher. Indeed, glutathione depletion strongly affected the viability of KO, but not of WT MEF, thereby indicating that oxidative stress is more elevated in KO MEF even though well controlled by glutathione. On the other hand, when cortical KO neurons were put in culture, they immediately appeared more vulnerable than WT to the acute oxidative stress condition, but after few days in vitro, the situation was reversed with KO neurons being more resistant than WT to acute stress. This compensatory, protective competence was not due to the upregulation of glutathione, rather of two mitochondrial antioxidant proteins: superoxide dismutase 2 and, at an even higher level, peroxiredoxin 3. This body of evidence sheds light on the capability of neurons to activate neuroprotective pathways and points the attention to peroxiredoxin 3, an antioxidant enzyme that might be critical for neuronal survival also in other disorders affecting mitochondria.

Published

2019

10. Pathogenic variants in the AFG3L2 proteolytic domain cause SCA28 through haploinsufficiency and proteostatic stress-driven OMA1 activation

Author

Cyril Goizet, Dagmar Nolte, Jonathan Baets, Tine Deconinck, Camilo Toro, Susanna Tulli, Valentina Baderna, Davide Mazza, Franca Codazzi, Peter DeJonghe, Alessandro Ambrosi, Giorgio Casari, Francesca Maltecca, Andrea Del Bondio, Tyler Mark Pierson, Paola Mandich, Tulli, S., Del Bondio, A., Baderna, V., Mazza, D., Codazzi, F., Pierson, T. M., Ambrosi, A., Nolte, D., Goizet, C., Toro, C., Baets, J., Deconinck, T., Dejonghe, P., Mandich, P., Casari, G., and Maltecca, F.

Subjects

0301 basic medicine, Haploinsufficiency, Mitochondrion, Medical and Health Sciences, Mice, 0302 clinical medicine, ATP-Dependent Proteases, Models, cell biology, molecular genetic, 2.1 Biological and endogenous factors, Missense mutation, genetics, Mitochondrial calcium uptake, Neurogenetics, Genetics (clinical), Genetics & Heredity, Mice, Knockout, Metalloendopeptidases, Biological Sciences, Mitochondria, Cell biology, mitochondria, mitochondrial fusion, Spinocerebellar ataxia, movement disorders (other than parkinsons), Protein Binding, Transcriptional Activation, Knockout, Physiological, Biology, Stress, Models, Biological, Frameshift mutation, molecular genetics, 03 medical and health sciences, Rare Diseases, Protein Domains, Stress, Physiological, Genetics, medicine, Animals, Humans, Genetic Variation, Fibroblasts, Biological, medicine.disease, HEK293 Cells, 030104 developmental biology, Proteostasis, Proteolysis, movement disorders, ATPases Associated with Diverse Cellular Activities, Calcium, Human medicine, Protein Multimerization, genetic, 030217 neurology & neurosurgery

Abstract

BackgroundSpinocerebellar ataxia type 28 (SCA28) is a dominantly inherited neurodegenerative disease caused by pathogenic variants in AFG3L2. The AFG3L2 protein is a subunit of mitochondrial m-AAA complexes involved in protein quality control. Objective of this study was to determine the molecular mechanisms of SCA28, which has eluded characterisation to date.MethodsWe derived SCA28 patient fibroblasts carrying different pathogenic variants in the AFG3L2 proteolytic domain (missense: the newly identified p.F664S and p.M666T, p.G671R, p.Y689H and a truncating frameshift p.L556fs) and analysed multiple aspects of mitochondrial physiology. As reference of residual m-AAA activity, we included SPAX5 patient fibroblasts with homozygous p.Y616C pathogenic variant, AFG3L2+/− HEK293 T cells by CRISPR/Cas9-genome editing and Afg3l2−/− murine fibroblasts.ResultsWe found that SCA28 cells carrying missense changes have normal levels of assembled m-AAA complexes, while the cells with a truncating pathogenic variant had only half of this amount. We disclosed inefficient mitochondrial fusion in SCA28 cells caused by increased OPA1 processing operated by hyperactivated OMA1. Notably, we found altered mitochondrial proteostasis to be the trigger of OMA1 activation in SCA28 cells, with pharmacological attenuation of mitochondrial protein synthesis resulting in stabilised levels of OMA1 and OPA1 long forms, which rescued mitochondrial fusion efficiency. Secondary to altered mitochondrial morphology, mitochondrial calcium uptake resulted decreased in SCA28 cells.ConclusionOur data identify the earliest events in SCA28 pathogenesis and open new perspectives for therapy. By identifying similar mitochondrial phenotypes between SCA28 cells and AFG3L2+/− cells, our results support haploinsufficiency as the mechanism for the studied pathogenic variants.

Published

2019

11. Intergenerational instability and marked anticipation in SCA-17

Author

A. Filla, Massimo Carella, Giovanni Coppola, Antonio Servadio, Giorgio Casari, N.A. Fragassi, Sergio Cocozza, Imma Castaldo, G. De Michele, Francesca Maltecca, Amalia C. Bruni, Maltecca, Francesca, Filla, A, Castaldo, I, Coppola, G, Fragassi, Na, Carella, M, Bruni, A, Cocozza, S, Casari, GIORGIO NEVIO, Servadio, A, De Michele, G., Maltecca, F, Filla, Alessandro, Cocozza, Sergio, Casari, G, and DE MICHELE, Giuseppe

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Ataxia, Adolescent, Epilepsy, Degenerative disease, medicine, Humans, Spinocerebellar Ataxias, Dementia, Anticipation, Genetic, TATA-Box Binding Protein, medicine.disease, Pedigree, Mutation, Anticipation (genetics), Spinocerebellar ataxia, Female, Cerebellar atrophy, Neurology (clinical), medicine.symptom, Trinucleotide Repeat Expansion, Trinucleotide repeat expansion, Psychology, Neuroscience

Abstract

The authors describe an Italian family with autosomal dominant ataxia, dementia, psychiatric and extrapyramidal features, epilepsy, mild sensorimotor axonal neuropathy, and MRI findings of cerebral and cerebellar atrophy. A child had a distinctive presentation with onset at 3 years, growth retardation, fast progression, and early death. Molecular analysis demonstrated an expanded CAG/CAA repeat in the TBP gene (SCA-17). The repeat size was 66 triplets in the child and 53 in all the other patients.

Published

2003

12. Behavioral disorder, dementia, ataxia, and rigidity in a large family with TATA box-binding protein mutation

Author

Giuseppe De Michele, Jean Francois Foncin, Raffaele Maletta, Francesca Maltecca, Amalia C. Bruni, Giorgio Casari, Junko Takahashi-Fujigasaki, Antonio Servadio, Khalid Hamid El Hachimi, Sabrina A.M. Curcio, Charles Duyckaerts, Alessandro Filla, Pio D’Adamo, Bruni, Ac, Takahashi Fujigasaki, J, Maltecca, F, Foncin, Jf, Servadio, A, Casari, GIORGIO NEVIO, D'Adamo, P, Maletta, R, Curcio, Sam, De Michele, G, Filla, A, El Hachimi, Kh, Duyckaerts, C., TAKAHASHI FUJIGASAKI, J, Casari, G, Dadamo, P, DE MICHELE, Giuseppe, Filla, Alessandro, EL HACHIMI, Kh, A. C., Bruni, J., Takahashi Fujigasaki, F., Maltecca, J. F., Foncin, A., Servadio, G., Casari, D'Adamo, ADAMO PIO, R., Maletta, S. a., M, Michele, G., A., Filla, K. H., El, and C., Duyckaerts

Subjects

Male, pathology [Spinocerebellar Ataxias], Pathology, Purkinje cell, Spinocerebellar Ataxias: pathology, Behavioral Symptoms, pathology [Dementia], psychology [Spinocerebellar Ataxias], Autosomal dominant cerebellar ataxia, pathology [Brain], Behavioral Symptoms: genetics, Muscle Rigidity: pathology, Muscle Rigidity: psychology, Dystonia, genetic [Dementia], Dementia: pathology, Brain, Middle Aged, Behavioral Symptoms: psychology, Pedigree, genetic [Spinocerebellar Ataxias], medicine.anatomical_structure, Dementia: genetics, psychology [Behavioral Symptoms], Spinocerebellar ataxia, Female, Cerebellar atrophy, medicine.symptom, Spinocerebellar Ataxias: psychology, Psychology, genetic [Behavioral Symptoms], Human, Adult, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Ataxia, psychology [Dementia], Behavioral Symptom, Spinocerebellar Ataxias: genetics, Dementia: psychology, pathology [Muscle Rigidity], Arts and Humanities (miscellaneous), psychology [Muscle Rigidity], medicine, Humans, Spinocerebellar Ataxias, Aged, Spinocerebellar Ataxia, Cerebellar ataxia, pathology [Behavioral Symptoms], Behavioral Symptoms: pathology, Brain: pathology, Dementia, Muscle Rigidity, Muscle Rigidity: genetics, Mutation, TATA-Box Binding Protein, TATA-Box Binding Protein: genetics, medicine.disease, genetics [TATA-Box Binding Protein], Neurology (clinical), genetic [Muscle Rigidity], Trinucleotide repeat expansion, Neuroscience

Abstract

Background Spinocerebellar ataxia type 17 is an autosomal dominant cerebellar ataxia caused by a CAG repeat expansion in the TATA box-binding protein gene. Ataxia is typically the first sign whereas behavioral symptoms occur later. Objective To characterize the unusual phenotypic expression of a large spinocerebellar ataxia type 17 kindred. Design Clinical, neuropathological, and molecular genetic characterization of a 4-generation family with 16 affected patients. Results Behavioral symptoms and frontal impairment dominated the early stages preceding ataxia, rigidity, and dystonic movements. Neuropathological examination showed cortical, subcortical, and cerebellar atrophy. Purkinje cell loss and gliosis, pseudohypertrophic degeneration of the inferior olive, marked neuronal loss and gliosis in the caudate nucleus, and in the medial thalamic nuclei were salient features together with neuronal intranuclear inclusions stained with anti–TATA box-binding protein and antipolyglutamine antibodies. The disease was caused by a stable 52 CAG repeat expansion of the TATA box-binding protein gene, although there was apparent variability in the age of onset. Conclusion The characteristics of this family broaden the clinical picture of spinocerebellar ataxia type 17: initial presenile dementia with behavioral symptoms should be added to ataxia, rigidity, and dystonic movements, which are more commonly encountered.

Published

2004

13. Genome-wide expression profiling and functional characterization of SCA28 lymphoblastoid cell lines reveal impairment in cell growth and activation of apoptotic pathways

Author

Luisa Iommarini, Ada Funaro, Stefano Gustincich, Anna Maria Porcelli, Giovanni Stevanin, Alessandro Brussino, Paola Roncaglia, Anna Bartoletti Stella, H Krmac, Giuseppe Gasparre, Cecilia Mancini, Francesca Maltecca, Claudia Cagnoli, Giorgio Casari, Isabelle Le Ber, Sylvie Forlani, Nicola Lo Buono, Maria Antonietta Calvaruso, Alfredo Brusco, Elena Gazzano, Alexandra Durr, Alexis Brice, Dario Ghigo, Mancini, C, Roncaglia, P, Brussino, A, Stevanin, G, Lo Buono, N, Krmac, H, Maltecca, Francesca, Gazzano, E, Stella, Ab, Calvaruso, Ma, Iommarini, L, Cagnoli, C, Forlani, S, Le Ber, I, Durr, A, Brice, A, Ghigo, D, Casari, GIORGIO NEVIO, Porcelli, Am, Funaro, A, Gasparre, G, Gustincich, S, Brusco, A., Department of Medical Sciences, Università degli studi di Torino = University of Turin (UNITO), Gene Ontology Editorial Office, European Bioinformatics Institute, Neurobiology Sector, Scuola Internazionale Superiore di Studi Avanzati / International School for Advanced Studies (SISSA / ISAS), CHU Pitié-Salpêtrière [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Centre de Recherche de l'Institut du Cerveau et de la Moelle épinière (CRICM), Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), San Raffaele Scientific Institute, Vita-Salute San Raffaele University and Center for Translational Genomics and Bioinformatics, Department of Oncology, Department Medical and Surgical Sciences, Medical Genetics, Alma Mater Studiorum Università di Bologna [Bologna] (UNIBO), Department of Pharmacy and Biotechnologies (FABIT), Medical Genetics Unit, 'Città della Salute e della Scienza' Hospital, This work was funded by Telethon Research grant GGP07110 and GGP12217 (to A Brusco), Regione Piemonte Ricerca Sanitaria Finalizzata, the European Union (to the EUROSCA consortium), the VERUM foundation (to A Brice) and the Programme Hospitalier de Recherche Clinique (to A Durr)., Università degli studi di Torino (UNITO), Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Centre National de la Recherche Scientifique (CNRS)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Pierre et Marie Curie - Paris 6 (UPMC), BMC, Ed., Mancini C, Roncaglia P, Brussino A, Stevanin G, Lo Buono N, Krmac H, Maltecca F, Gazzano E, Bartoletti Stella A, Calvaruso MA, Iommarini L, Cagnoli C, Forlani S, Le Ber I, Durr A, Brice A, Ghigo D, Casari G, Porcelli AM, Funaro A, Gasparre G, Gustincich S, and Brusco A

Subjects

Respiratory chain, Apoptosis, Gene mutation, GTP Phosphohydrolases, 0302 clinical medicine, ATP-Dependent Proteases, Settore BIO/13 - Biologia Applicata, Gene expression, Genetics(clinical), Autosomal dominant cerebellar ataxia, Spinocerebellar ataxia, SCA28, AFG3L2, Genome-wide expression, LCLs, Genetics (clinical), Spinocerebellar Degenerations, 0303 health sciences, Cell biology, Mitochondria, ataxia, mitochondria, DNA-Binding Proteins, Phenotype, [SDV.BBM.GTP] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Genomics [q-bio.GN], Chemical homeostasis, Microtubule-Associated Proteins, Research Article, Dynamins, Biology, Mitochondrial Proteins, 03 medical and health sciences, [SDV.BBM.GTP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Genomics [q-bio.GN], Cell Line, Tumor, Genetics, Humans, Spinocerebellar Ataxias, Gene, 030304 developmental biology, Cell Proliferation, Cell growth, Genome, Human, Gene Expression Profiling, TFAM, Molecular biology, G1 Phase Cell Cycle Checkpoints, Gene expression profiling, ATPases Associated with Diverse Cellular Activities, Lipid Peroxidation, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Background SCA28 is an autosomal dominant ataxia associated with AFG3L2 gene mutations. We performed a whole genome expression profiling using lymphoblastoid cell lines (LCLs) from four SCA28 patients and six unrelated healthy controls matched for sex and age. Methods Gene expression was evaluated with the Affymetrix GeneChip Human Genome U133A 2.0 Arrays and data were validated by real-time PCR. Results We found 66 genes whose expression was statistically different in SCA28 LCLs, 35 of which were up-regulated and 31 down-regulated. The differentially expressed genes were clustered in five functional categories: (1) regulation of cell proliferation; (2) regulation of programmed cell death; (3) response to oxidative stress; (4) cell adhesion, and (5) chemical homeostasis. To validate these data, we performed functional experiments that proved an impaired SCA28 LCLs growth compared to controls (p Conclusions Whole genome expression profiling, performed on SCA28 LCLs, allowed us to identify five altered functional categories that characterize the SCA28 LCLs phenotype, the first reported in human cells to our knowledge.

14. Clinical-grade intranasal NGF fuels neurological and metabolic functions of Mecp2-deficient mice.

Author

Pozzer D, Indrigo M, Breccia M, Florio E, Franchino CA, De Rocco G, Maltecca F, Fadda A, Rossato M, Aramini A, Allegretti M, Frasca A, De Filippis L, and Landsberger N

Subjects

Animals, Male, Mice, Female, Mice, Knockout, Disease Models, Animal, Humans, Mice, Inbred C57BL, Recombinant Proteins pharmacology, Recombinant Proteins administration & dosage, Methyl-CpG-Binding Protein 2 genetics, Nerve Growth Factor metabolism, Administration, Intranasal, Rett Syndrome drug therapy, Rett Syndrome genetics

Abstract

MECP2 deficiency causes a broad spectrum of neuropsychiatric disorders that can affect both genders. Rett syndrome is the most common and is characterized by an apparently normal growth period followed by a regression phase in which patients lose most of their previously acquired skills. After this dramatic period, various symptoms progressively appear, including severe intellectual disability, epilepsy, apraxia, breathing abnormalities and motor deterioration. MECP2 encodes for an epigenetic transcription factor that is particularly abundant in the brain; consequently, several transcriptional defects characterize the Rett syndrome brain. The well-known deficiency of several neurotrophins and growth factors, together with the positive effects exerted by trofinetide, a synthetic analogue of insulin-like growth factor 1, in Rett patients and in mouse models of Mecp2 deficiency, prompted us to investigate the therapeutic potential of nerve growth factor. Initial in vitro studies demonstrated a healing effect of recombinant human GMP-grade NGF (rhNGF) on neuronal maturation and activity in cultured Mecp2-null neurons. Subsequently, we designed in vivo studies with clear translational potential using intranasally administered rhNGF already used in the clinic. The efficacy of rhNGF in vivo in Mecp2-null hemizygous male mice and heterozygous female mice was assessed. General well-being was evaluated by a conventional phenotypic score and motor performance through the Pole and Beam Walking tests, while cognitive function and interaction with the environment were measured by the Novel Object Recognition test and the Marble Burying test, respectively. At the end of the treatment, mouse cortices were dissected and bulk RNA sequencing was performed to identify the molecular pathways involved in the protective effects of rhNGF. In both male and female mouse models of Rett syndrome, rhNGF exerted positive effects on cognitive and motor functions. In male hemizygous mice, which suffer from significantly more severe and rapidly advancing symptoms, the drug's ability to slow the disease's progression was more pronounced. The unbiased research for the molecular mechanisms triggering the observed benefits revealed a strong positive effect on gene sets related to oxidative phosphorylation, mitochondrial structure and function. These results were validated by demonstrating the drug's ability to improve mitochondrial structure and respiration in Mecp2-null cerebral cortices. Furthermore, Gene Ontology analyses indicated that NGF exerted the expected improvement in neuronal maturation. We conclude that intranasal administration of rhNGF is a non-invasive and effective route of administration for the treatment of Rett syndrome and possibly for other neurometabolic disorders with overt mitochondrial dysfunction., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2025

15. Longitudinal Imaging Biomarkers Correlate with Progressive Motor Deficit in the Mouse Model of Charlevoix-Saguenay Ataxia.

Author

Gigliucci V, Huang SC, Boschetti G, Scaravilli A, Castoldi V, Podini P, Quattrini A, Cocozza S, Leocani L, and Maltecca F

Subjects

Animals, Mice, Retina diagnostic imaging, Retina pathology, Biomarkers, Longitudinal Studies, Brain diagnostic imaging, Brain pathology, Male, Mice, Knockout, Mice, Inbred C57BL, Tomography, Optical Coherence methods, Disease Models, Animal, Disease Progression, Magnetic Resonance Imaging, Muscle Spasticity diagnostic imaging, Muscle Spasticity physiopathology, Muscle Spasticity genetics, Spinocerebellar Ataxias diagnostic imaging, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias physiopathology, Spinocerebellar Ataxias congenital

Abstract

Objective: In autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) disease, severity and age of onset vary greatly, hindering to objectively measure and predict clinical progression. Thickening of the retinal nerve fiber layer is distinctive of ARSACS patients, as assessed by optical coherence tomography, whereas conventional brain magnetic resonance imaging findings include both supratentorial and infratentorial changes. Because longitudinal imaging studies in ARSACS patients are not available to define these changes as biomarkers of disease progression, we aimed to address this issue in the ARSACS mouse model., Methods: We performed longitudinal retinal OCT and brain MRI in the Sacs -/- ARSACS mouse model, alongside motor and coordination assessment in the beam walking test. We also investigated visual function and the molecular mechanisms underlying RNFL increased thickness by histology and immunofluorescence., Results: We demonstrated that RNFL thickening by OCT gradually increases in the early stages of pathology in the Sacs -/- mouse model, reflecting the progression of motor impairment, and later reaches a plateau when thinning of the posterior corpus callosum becomes detectable by MRI. Mechanistically, we unveiled that RNFL thickening is associated with aberrant accumulation of non-phosphorylated neurofilament H and glial fibrillary acidic protein. We also uncovered mild signs of myelin pathology coherent with increased latency of visual evoked potentials, and altered retinal activation by photopic electroretinography., Interpretation: We show that both RNFL thickening and MRI changes may represent biomarkers of disease progression in the Sacs -/- mouse model. Our data gathers knowledge instrumental to clinical studies, holding potential as readout for treatment efficacy. ANN NEUROL 2025;97:425-434., (© 2024 The Author(s). Annals of Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association.)

Published

2025

16. Reduction of sacsin levels in peripheral blood mononuclear cells as a diagnostic tool for spastic ataxia of Charlevoix-Saguenay.

Author

De Ritis D, Ferrè L, De Winter J, Tremblay-Desbiens C, Blais M, Bassi MT, Dupré N, Baets J, Filippi M, and Maltecca F

Abstract

Autosomal recessive spastic ataxia of Charlevoix-Saguenay is a rare neurodegenerative disease caused by biallelic variants in the SACS gene encoding for sacsin. More than 200 pathogenic variants have been identified to date, most of which are missense. It is likely that the prevalence of autosomal recessive spastic ataxia of Charlevoix-Saguenay is underestimated due to the lack of an efficient diagnostic tool able to validate variants of uncertain significance. We have previously shown that sacsin is almost absent in fibroblasts of patients with autosomal recessive spastic ataxia of Charlevoix-Saguenay regardless of the type of SACS variant, because sacsin carrying missense variants is cotranslationally degraded. In this work, we aimed to establish the pathogenicity of SACS variants by quantifying sacsin protein in blood samples, with relevant implications for autosomal recessive spastic ataxia of Charlevoix-Saguenay diagnosis. We developed a protocol to assess sacsin protein levels by western blot using small amounts of peripheral blood mononuclear cells, which can be propagated in culture and cryopreserved. The study involves eight patients with autosomal recessive spastic ataxia of Charlevoix-Saguenay (including a novel case) carrying variants of different types and positions along the SACS gene and two parents who are carriers of heterozygous missense variants. We show that patients with autosomal recessive spastic ataxia of Charlevoix-Saguenay (carrying either missense or truncating variants) almost completely lacked sacsin in peripheral blood mononuclear cells. Moreover, both carriers of a SACS missense variant showed 50% reduction in sacsin protein levels compared to controls. We also describe a patient with uniparental isodisomy carrying a homozygous nonsense variant near the 3' end of the SACS gene. This resulted in a stable sacsin protein lacking the last 202 amino acids, probably due to escape of nonsense-mediated decay of mRNA. In conclusion, we have optimized a minimally invasive diagnostic tool for autosomal recessive spastic ataxia of Charlevoix-Saguenay in blood samples based on sacsin protein level assessment. Indeed, our results provide definite evidence that sacsin carrying missense pathogenic variants undergoes cotranslational degradation. The quantitative reduction in sacsin levels in the case of missense variants of uncertain significance allows defining them as pathogenic variants, something which cannot be predicted bioinformatically with high certainty., Competing Interests: The authors report no competing interests., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2024

17. Sustained OMA1-mediated integrated stress response is beneficial for spastic ataxia type 5.

Author

Franchino CA, Brughera M, Baderna V, De Ritis D, Rocco A, Seneca S, Regal L, Podini P, D'Antonio M, Toro C, Quattrini A, Scalais E, and Maltecca F

Subjects

Humans, Animals, Mice, Child, Muscle Spasticity, Peptide Hydrolases, ATPases Associated with Diverse Cellular Activities genetics, ATP-Dependent Proteases genetics, Mitochondrial Proteins, Metalloproteases, Spinocerebellar Ataxias genetics, Optic Atrophy, Intellectual Disability

Abstract

AFG3L2 is a mitochondrial protease exerting protein quality control in the inner mitochondrial membrane. Heterozygous AFG3L2 mutations cause spinocerebellar ataxia type 28 (SCA28) or dominant optic atrophy type 12 (DOA12), while biallelic AFG3L2 mutations result in the rare and severe spastic ataxia type 5 (SPAX5). The clinical spectrum of SPAX5 includes childhood-onset cerebellar ataxia, spasticity, dystonia and myoclonic epilepsy. We previously reported that the absence or mutation of AFG3L2 leads to the accumulation of mitochondria-encoded proteins, causing the overactivation of the stress-sensitive protease OMA1, which over-processes OPA1, leading to mitochondrial fragmentation. Recently, OMA1 has been identified as the pivotal player communicating mitochondrial stress to the cytosol via a pathway involving the inner mitochondrial membrane protein DELE1 and the cytosolic kinase HRI, thus eliciting the integrated stress response. In general, the integrated stress response reduces global protein synthesis and drives the expression of cytoprotective genes that allow cells to endure proteotoxic stress. However, the relevance of the OMA1-DELE1-HRI axis in vivo, and especially in a human CNS disease context, has been poorly documented thus far. In this work, we demonstrated that mitochondrial proteotoxicity in the absence/mutation of AFG3L2 activates the OMA1-DELE1-HRI pathway eliciting the integrated stress response. We found enhanced OMA1-dependent processing of DELE1 upon depletion of AFG3L2. Also, in both skin fibroblasts from SPAX5 patients (including a novel case) and in the cerebellum of Afg3l2-/- mice we detected increased phosphorylation of the α-subunit of the eukaryotic translation initiation factor 2 (eIF2α), increased levels of ATF4 and strong upregulation of its downstream targets (Chop, Chac1, Ppp1r15a and Ffg21). Silencing of DELE1 or HRI in SPAX5 fibroblasts (where OMA1 is overactivated at basal state) reduces eIF2α phosphorylation and affects cell growth. In agreement, pharmacological potentiation of integrated stress response via Sephin-1, a drug that selectively inhibits the stress-induced eIF2alpha phosphatase GADD34 (encoded by Ppp1r15a), improved cell growth of SPAX5 fibroblasts and cell survival and dendritic arborization ex vivo in primary Afg3l2-/- Purkinje neurons. Notably, Sephin-1 treatment in vivo extended the lifespan of Afg3l2-/- mice, improved Purkinje neuron morphology, mitochondrial ultrastructure and respiratory capacity. These data indicate that activation of the OMA1-DELE1-HRI pathway is protective in the context of SPAX5. Pharmacological tuning of the integrated stress response may represent a future therapeutic strategy for SPAX5 and other cerebellar ataxias caused by impaired mitochondrial proteostasis., (© The Author(s) 2023. Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2024

18. Restoring calcium homeostasis in Purkinje cells arrests neurodegeneration and neuroinflammation in the ARSACS mouse model.

Author

Del Bondio A, Longo F, De Ritis D, Spirito E, Podini P, Brais B, Bachi A, Quattrini A, and Maltecca F

Subjects

Muscle Spasticity, Neuroinflammatory Diseases, Spinocerebellar Ataxias congenital, Heat-Shock Proteins genetics, Mice, Ceftriaxone metabolism, Animals, Calcium metabolism, Purkinje Cells metabolism

Abstract

Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) is caused by mutations in SACS gene encoding sacsin, a huge protein highly expressed in cerebellar Purkinje cells (PCs). Patients with ARSACS, as well as mouse models, display early degeneration of PCs, but the underlying mechanisms remain unexplored, with no available treatments. In this work, we demonstrated aberrant calcium (Ca2+) homeostasis and its impact on PC degeneration in ARSACS. Mechanistically, we found pathological elevation in Ca2+-evoked responses in Sacs-/- PCs as the result of defective mitochondria and ER trafficking to distal dendrites and strong downregulation of key Ca2+ buffer proteins. Alteration of cytoskeletal linkers, which we identified as specific sacsin interactors, likely account for faulty organellar trafficking in Sacs-/- cerebellum. Based on this pathogenetic cascade, we treated Sacs-/- mice with Ceftriaxone, a repurposed drug that exerts neuroprotection by limiting neuronal glutamatergic stimulation and, thus, Ca2+ fluxes into PCs. Ceftriaxone treatment significantly improved motor performances of Sacs-/- mice, at both pre- and postsymptomatic stages. We correlated this effect to restored Ca2+ homeostasis, which arrests PC degeneration and attenuates secondary neuroinflammation. These findings disclose key steps in ARSACS pathogenesis and support further optimization of Ceftriaxone in preclinical and clinical settings for the treatment of patients with ARSACS.

Published

2023

19. SETD5 haploinsufficiency affects mitochondrial compartment in neural cells.

Author

Zaghi M, Longo F, Massimino L, Rubio A, Bido S, Mazzara PG, Bellini E, Banfi F, Podini P, Maltecca F, Zippo A, Broccoli V, and Sessa A

Subjects

Mice, Animals, Humans, Neurons metabolism, Mitochondria metabolism, Chromatin metabolism, Methyltransferases genetics, Methyltransferases metabolism, Haploinsufficiency, Neural Stem Cells metabolism

Abstract

Background: Neurodevelopmental disorders (NDDs) are heterogeneous conditions due to alterations of a variety of molecular mechanisms and cell dysfunctions. SETD5 haploinsufficiency leads to NDDs due to chromatin defects. Epigenetic basis of NDDs has been reported in an increasing number of cases while mitochondrial dysfunctions are more common within NDD patients than in the general population., Methods: We investigated in vitro neural stem cells as well as the brain of the Setd5 haploinsufficiency mouse model interrogating its transcriptome, analyzing mitochondrial structure, biochemical composition, and dynamics, as well as mitochondrial functionality., Results: Mitochondrial impairment is facilitated by transcriptional aberrations originated by the decrease of the SETD5 enzyme. Low levels of SETD5 resulted in fragmented mitochondria, reduced mitochondrial membrane potential, and ATP production both in neural precursors and neurons. Mitochondria were also mislocalized in mutant neurons, with reduced organelles within neurites and synapses., Limitations: We found several defects in the mitochondrial compartment; however, we can only speculate about their position in the hierarchy of the pathological mechanisms at the basis of the disease., Conclusions: Our study explores the interplay between chromatin regulation and mitochondria functions as a possible important aspect of SETD5-associated NDD pathophysiology. Our data, if confirmed in patient context, suggest that the mitochondrial activity and dynamics may represent new therapeutic targets for disorders associated with the loss of SETD5., (© 2023. The Author(s).)

Published

2023

20. Assessment of Sacsin Turnover in Patients With ARSACS: Implications for Molecular Diagnosis and Pathogenesis.

Author

Longo F, De Ritis D, Miluzio A, Fraticelli D, Baets J, Scarlato M, Santorelli FM, Biffo S, and Maltecca F

Subjects

Ataxia genetics, Humans, Muscle Spasticity diagnosis, Muscle Spasticity genetics, Mutation genetics, Heat-Shock Proteins genetics, Heat-Shock Proteins metabolism, Spinocerebellar Ataxias congenital, Spinocerebellar Ataxias diagnosis, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias pathology

Abstract

Background and Objectives: Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) is caused by variations in SACS gene encoding sacsin, a huge multimodular protein of unknown function. More than 200 SACS variations have been described worldwide to date. Because ARSACS presents phenotypic variability, previous empirical studies attempted to correlate the nature and position of SACS variations with the age at onset or with disease severity, although not considering the effect of the various variations on protein stability. In this work, we studied genotype-phenotype correlation in ARSACS at a functional level., Methods: We analyzed a large set of skin fibroblasts derived from patients with ARSACS, including both new and already published cases, carrying variations of different types affecting diverse domains of the protein., Results: We found that sacsin is almost absent in patients with ARSACS, regardless of the nature of the variation. As expected, we did not detect sacsin in patients with truncating variations. We found it strikingly reduced or absent also in compound heterozygotes carrying diverse missense variations. In this case, we excluded SACS mRNA decay, defective translation, or faster posttranslational degradation as possible causes of protein reduction. Conversely, our results demonstrate that nascent mutant sacsin protein undergoes cotranslational ubiquitination and degradation., Discussion: Our results provide a mechanistic explanation for the lack of genotype-phenotype correlation in ARSACS. We also propose a new and unambiguous criterion for ARSACS diagnosis that is based on the evaluation of sacsin level. Last, we identified preemptive degradation of a mutant protein as a novel cause of a human disease., (Copyright © 2021 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published

2021

21. U-Fiber Leukoencephalopathy Due to a Novel Mutation in the TACO1 Gene.

Author

Sferruzza G, Del Bondio A, Citterio A, Vezzulli P, Guerrieri S, Radaelli M, Martinelli Boneschi F, Filippi M, Maltecca F, Bassi MT, and Scarlato M

Published

2021

22. A novel AFG3L2 mutation close to AAA domain leads to aberrant OMA1 and OPA1 processing in a family with optic atrophy.

Author

Baderna V, Schultz J, Kearns LS, Fahey M, Thompson BA, Ruddle JB, Huq A, and Maltecca F

Subjects

AAA Domain genetics, Adolescent, Child, Child, Preschool, Female, GTP Phosphohydrolases metabolism, Humans, Male, Metalloendopeptidases metabolism, Mutation, Missense, Pedigree, ATP-Dependent Proteases genetics, ATPases Associated with Diverse Cellular Activities genetics, Optic Atrophy, Autosomal Dominant genetics, Optic Atrophy, Autosomal Dominant metabolism

Abstract

Autosomal dominant optic atrophy (ADOA) is a neuro-ophthalmic condition characterized by bilateral degeneration of the optic nerves. Although heterozygous mutations in OPA1 represent the most common genetic cause of ADOA, a significant number of cases remain undiagnosed.Here, we describe a family with a strong ADOA history with most family members spanning three generation having childhood onset of visual symptoms. The proband, in addition to optic atrophy, had neurological symptoms consistent with relapsing remitting multiple sclerosis. Clinical exome analysis detected a novel mutation in the AFG3L2 gene (NM_006796.2:c.1010G > A; p.G337E), which segregated with optic atrophy in family members. AFG3L2 is a metalloprotease of the AAA subfamily which exerts quality control in the inner mitochondrial membrane. Interestingly, the identified mutation localizes close to the AAA domain of AFG3L2, while those localized in the proteolytic domain cause dominant spinocerebellar ataxia type 28 (SCA28) or recessive spastic ataxia with epilepsy (SPAX5). Functional studies in patient fibroblasts demonstrate that the p.G337E AFG3L2 mutation strongly destabilizes the long isoforms of OPA1 via OMA hyper-activation and leads to mitochondrial fragmentation, thus explaining the family phenotype. This study widens the clinical spectrum of neurodegenerative diseases caused by AFG3L2 mutations, which shall be considered as genetic cause of ADOA.

Published

2020

23. Impaired turnover of hyperfused mitochondria in severe axonal neuropathy due to a novel DRP1 mutation.

Author

Longo F, Benedetti S, Zambon AA, Sora MGN, Di Resta C, De Ritis D, Quattrini A, Maltecca F, Ferrari M, and Previtali SC

Subjects

Autophagy genetics, Child, Preschool, Dynamins metabolism, Female, Fibroblasts cytology, Fibroblasts metabolism, Heterozygote, Humans, Mitochondria metabolism, Mitochondria pathology, Mutation, Pedigree, Peripheral Nervous System Diseases enzymology, Peripheral Nervous System Diseases metabolism, Peripheral Nervous System Diseases pathology, Peroxisomes metabolism, Reactive Oxygen Species metabolism, Exome Sequencing, Dynamins genetics, Fibroblasts ultrastructure, Mitochondria genetics, Mitochondria ultrastructure, Mitochondrial Dynamics genetics, Peripheral Nervous System Diseases genetics

Abstract

Mitochondria undergo continuous cycles of fusion and fission in response to physiopathological stimuli. The key player in mitochondrial fission is dynamin-related protein 1 (DRP1), a cytosolic protein encoded by dynamin 1-like (DNM1L) gene, which relocalizes to the outer mitochondrial membrane, where it assembles, oligomerizes and drives mitochondrial division upon guanosine-5'-triphosphate (GTP) hydrolysis. Few DRP1 mutations have been described so far, with patients showing complex and variable phenotype ranging from early death to encephalopathy and/or optic atrophy. The disease is the consequence of defective mitochondrial fission due to faulty DRP1 function. However, the underlying molecular mechanisms and the functional consequences at mitochondrial and cellular level remain elusive. Here we report on a 5-year-old girl presenting psychomotor developmental delay, global hypotonia and severe ataxia due to axonal sensory neuropathy harboring a novel de novo heterozygous missense mutation in the GTPase domain of DRP1 (NM_012062.3:c.436G>A, NP_036192.2: p.D146N variant in DNM1L). Patient's fibroblasts show hyperfused/balloon-like giant mitochondria, highlighting the importance of D146 residue for DRP1 function. This dramatic mitochondrial rearrangement phenocopies what observed overexpressing DRP1-K38A, a well-known experimental dominant negative version of DRP1. In addition, we demonstrated that p.D146N mutation has great impact on peroxisomal shape and function. The p.D146N mutation compromises the GTPase activity without perturbing DRP1 recruitment or assembly, causing decreased mitochondrial and peroxisomal turnover. In conclusion, our findings highlight the importance of sensory neuropathy in the clinical spectrum of DRP1 variants and, for the first time, the impact of DRP1 mutations on mitochondrial turnover and peroxisomal functionality., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2020

24. The WRB Subunit of the Get3 Receptor is Required for the Correct Integration of its Partner CAML into the ER.

Author

Carvalho HJF, Del Bondio A, Maltecca F, Colombo SF, and Borgese N

Subjects

Adaptor Proteins, Signal Transducing chemistry, Arsenite Transporting ATPases chemistry, Biomarkers, Fluorescent Antibody Technique, Humans, Membrane Proteins chemistry, Membrane Proteins metabolism, Proteasome Endopeptidase Complex metabolism, Protein Binding, Protein Transport, Proteolysis, Adaptor Proteins, Signal Transducing metabolism, Arsenite Transporting ATPases metabolism, Endoplasmic Reticulum metabolism, Protein Interaction Domains and Motifs

Abstract

Calcium-modulating cyclophilin ligand (CAML), together with Tryptophan rich basic protein (WRB, Get1 in yeast), constitutes the mammalian receptor for the Transmembrane Recognition Complex subunit of 40 kDa (TRC40, Get3 in yeast), a cytosolic ATPase with a central role in the post-translational targeting pathway of tail-anchored (TA) proteins to the endoplasmic reticulum (ER) membrane. CAML has also been implicated in other cell-specific processes, notably in immune cell survival, and has been found in molar excess over WRB in different cell types. Notwithstanding the stoichiometric imbalance, WRB and CAML depend strictly on each other for expression. Here, we investigated the mechanism by which WRB impacts CAML levels. We demonstrate that CAML, generated in the presence of sufficient WRB levels, is inserted into the ER membrane with three transmembrane segments (TMs) in its C-terminal region. By contrast, without sufficient levels of WRB, CAML fails to adopt this topology, and is instead incompletely integrated to generate two aberrant topoforms; these congregate in ER-associated clusters and are degraded by the proteasome. Our results suggest that WRB, a member of the recently proposed Oxa1 superfamily, acts catalytically to assist the topogenesis of CAML and may have wider functions in membrane biogenesis than previously appreciated.

Published

2019

25. Pathogenic variants in the AFG3L2 proteolytic domain cause SCA28 through haploinsufficiency and proteostatic stress-driven OMA1 activation.

Author

Tulli S, Del Bondio A, Baderna V, Mazza D, Codazzi F, Pierson TM, Ambrosi A, Nolte D, Goizet C, Toro C, Baets J, Deconinck T, DeJonghe P, Mandich P, Casari G, and Maltecca F

Subjects

ATP-Dependent Proteases chemistry, ATP-Dependent Proteases metabolism, ATPases Associated with Diverse Cellular Activities chemistry, ATPases Associated with Diverse Cellular Activities metabolism, Animals, Calcium metabolism, Fibroblasts metabolism, HEK293 Cells, Humans, Metalloendopeptidases metabolism, Mice, Mice, Knockout, Mitochondria genetics, Mitochondria metabolism, Models, Biological, Protein Binding, Protein Multimerization, Proteolysis, Proteostasis genetics, Transcriptional Activation, ATP-Dependent Proteases genetics, ATPases Associated with Diverse Cellular Activities genetics, Genetic Variation, Haploinsufficiency, Metalloendopeptidases genetics, Protein Domains genetics, Stress, Physiological genetics

Abstract

Background: Spinocerebellar ataxia type 28 (SCA28) is a dominantly inherited neurodegenerative disease caused by pathogenic variants in AFG3L2. The AFG3L2 protein is a subunit of mitochondrial m -AAA complexes involved in protein quality control. Objective of this study was to determine the molecular mechanisms of SCA28, which has eluded characterisation to date., Methods: We derived SCA28 patient fibroblasts carrying different pathogenic variants in the AFG3L2 proteolytic domain (missense: the newly identified p.F664S and p.M666T, p.G671R, p.Y689H and a truncating frameshift p.L556fs) and analysed multiple aspects of mitochondrial physiology. As reference of residual m -AAA activity, we included SPAX5 patient fibroblasts with homozygous p.Y616C pathogenic variant, AFG3L2 +/- HEK293 T cells by CRISPR/Cas9-genome editing and Afg3l2 -/- murine fibroblasts., Results: We found that SCA28 cells carrying missense changes have normal levels of assembled m -AAA complexes, while the cells with a truncating pathogenic variant had only half of this amount. We disclosed inefficient mitochondrial fusion in SCA28 cells caused by increased OPA1 processing operated by hyperactivated OMA1. Notably, we found altered mitochondrial proteostasis to be the trigger of OMA1 activation in SCA28 cells, with pharmacological attenuation of mitochondrial protein synthesis resulting in stabilised levels of OMA1 and OPA1 long forms, which rescued mitochondrial fusion efficiency. Secondary to altered mitochondrial morphology, mitochondrial calcium uptake resulted decreased in SCA28 cells., Conclusion: Our data identify the earliest events in SCA28 pathogenesis and open new perspectives for therapy. By identifying similar mitochondrial phenotypes between SCA28 cells and AFG3L2 +/- cells, our results support haploinsufficiency as the mechanism for the studied pathogenic variants., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2019. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2019

26. Mice harbouring a SCA28 patient mutation in AFG3L2 develop late-onset ataxia associated with enhanced mitochondrial proteotoxicity.

Author

Mancini C, Hoxha E, Iommarini L, Brussino A, Richter U, Montarolo F, Cagnoli C, Parolisi R, Gondor Morosini DI, Nicolò V, Maltecca F, Muratori L, Ronchi G, Geuna S, Arnaboldi F, Donetti E, Giorgio E, Cavalieri S, Di Gregorio E, Pozzi E, Ferrero M, Riberi E, Casari G, Altruda F, Turco E, Gasparre G, Battersby BJ, Porcelli AM, Ferrero E, Brusco A, and Tempia F

Subjects

Animals, Female, Gene Knock-In Techniques, Membrane Potential, Mitochondrial, Mice, Inbred C57BL, Mitochondrial Proteins metabolism, Mutation, Missense, Purkinje Cells physiology, Purkinje Cells ultrastructure, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias metabolism, Spinocerebellar Ataxias pathology, ATP-Dependent Proteases genetics, ATPases Associated with Diverse Cellular Activities genetics, Disease Models, Animal, Mitochondria metabolism, Spinocerebellar Ataxias congenital

Abstract

Spinocerebellar ataxia 28 is an autosomal dominant neurodegenerative disorder caused by missense mutations affecting the proteolytic domain of AFG3L2, a major component of the mitochondrial m-AAA protease. However, little is known of the underlying pathogenetic mechanisms or how to treat patients with SCA28. Currently available Afg3l2 mutant mice harbour deletions that lead to severe, early-onset neurological phenotypes that do not faithfully reproduce the late-onset and slowly progressing SCA28 phenotype. Here we describe production and detailed analysis of a new knock-in murine model harbouring an Afg3l2 allele carrying the p.Met665Arg patient-derived mutation. Heterozygous mutant mice developed normally but adult mice showed signs of cerebellar ataxia detectable by beam test. Although cerebellar pathology was negative, electrophysiological analysis showed a trend towards increased spontaneous firing in Purkinje cells from heterozygous mutants with respect to wild-type controls. As homozygous mutants died perinatally with evidence of cardiac atrophy, for each genotype we generated mouse embryonic fibroblasts (MEFs) to investigate mitochondrial function. MEFs from mutant mice showed altered mitochondrial bioenergetics, with decreased basal oxygen consumption rate, ATP synthesis and mitochondrial membrane potential. Mitochondrial network formation and morphology was altered, with greatly reduced expression of fusogenic Opa1 isoforms. Mitochondrial alterations were also detected in cerebella of 18-month-old heterozygous mutants and may be a hallmark of disease. Pharmacological inhibition of de novo mitochondrial protein translation with chloramphenicol caused reversal of mitochondrial morphology in homozygous mutant MEFs, supporting the relevance of mitochondrial proteotoxicity for SCA28 pathogenesis and therapy development., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2019

27. m-AAA and i-AAA complexes coordinate to regulate OMA1, the stress-activated supervisor of mitochondrial dynamics.

Author

Consolato F, Maltecca F, Tulli S, Sambri I, and Casari G

Subjects

ATP-Dependent Proteases chemistry, ATPases Associated with Diverse Cellular Activities chemistry, Apoptosis genetics, Consensus Sequence genetics, GTP Phosphohydrolases chemistry, HeLa Cells, Humans, Mitochondria chemistry, Mitochondrial Dynamics genetics, Mitochondrial Membranes chemistry, Mitochondrial Membranes metabolism, Mitochondrial Proteins genetics, Protein Processing, Post-Translational genetics, Proteolysis, ATP-Dependent Proteases genetics, ATPases Associated with Diverse Cellular Activities genetics, GTP Phosphohydrolases genetics, Metalloendopeptidases genetics, Mitochondria genetics

Abstract

The proteolytic processing of dynamin-like GTPase OPA1, mediated by the activity of both YME1L1 [intermembrane (i)-AAA protease complex] and OMA1, is a crucial step in the regulation of mitochondrial dynamics. OMA1 is a zinc metallopeptidase of the inner mitochondrial membrane that undergoes pre-activating proteolytic and auto-proteolytic cleavage after mitochondrial import. Here, we identify AFG3L2 [matrix (m) - AAA complex] as the major protease mediating this event, which acts by maturing the 60 kDa pre-pro-OMA1 to the 40 kDa pro-OMA1 form by severing the N-terminal portion without recognizing a specific consensus sequence. Therefore, m - AAA and i - AAA complexes coordinately regulate OMA1 processing and turnover, and consequently control which OPA1 isoforms are present, thus adding new information on the molecular mechanisms of mitochondrial dynamics and neurodegenerative diseases affected by these phenomena.This article has an associated First Person interview with the first author of the paper., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2018. Published by The Company of Biologists Ltd.)

Published

2018

28. Altered organization of the intermediate filament cytoskeleton and relocalization of proteostasis modulators in cells lacking the ataxia protein sacsin.

Author

Duncan EJ, Larivière R, Bradshaw TY, Longo F, Sgarioto N, Hayes MJ, Romano LEL, Nethisinghe S, Giunti P, Bruntraeger MB, Durham HD, Brais B, Maltecca F, Gentil BJ, and Chapple JP

Subjects

Animals, Ataxia genetics, Cell Culture Techniques, Cytoskeleton metabolism, Fibroblasts metabolism, HSP70 Heat-Shock Proteins metabolism, Heat-Shock Proteins genetics, Humans, Lysosomal-Associated Membrane Protein 2 metabolism, Mice, Mitochondria metabolism, Molecular Chaperones metabolism, Muscle Spasticity genetics, Muscle Spasticity metabolism, Proteostasis genetics, Proteostasis physiology, RNA-Binding Proteins metabolism, Spinocerebellar Ataxias congenital, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias metabolism, Vimentin metabolism, Heat-Shock Proteins metabolism, Intermediate Filaments metabolism

Abstract

Autosomal Recessive Spastic Ataxia of Charlevoix-Saguenay (ARSACS) is caused by mutations in the gene SACS, encoding the 520 kDa protein sacsin. Although sacsin's physiological role is largely unknown, its sequence domains suggest a molecular chaperone or protein quality control function. Consequences of its loss include neurofilament network abnormalities, specifically accumulation and bundling of perikaryal and dendritic neurofilaments. To investigate if loss of sacsin affects intermediate filaments more generally, the distribution of vimentin was analysed in ARSACS patient fibroblasts and in cells where sacsin expression was reduced. Abnormal perinuclear accumulation of vimentin filaments, which sometimes had a cage-like appearance, occurred in sacsin-deficient cells. Mitochondria and other organelles were displaced to the periphery of vimentin accumulations. Reorganization of the vimentin network occurs in vitro under stress conditions, including when misfolded proteins accumulate. In ARSACS patient fibroblasts HSP70, ubiquitin and the autophagy-lysosome pathway proteins Lamp2 and p62 relocalized to the area of the vimentin accumulation. There was no overall increase in ubiquitinated proteins, suggesting the ubiquitin-proteasome system was not impaired. There was evidence for alterations in the autophagy-lysosome pathway. Specifically, in ARSACS HDFs cellular levels of Lamp2 were elevated while levels of p62, which is degraded in autophagy, were decreased. Moreover, autophagic flux was increased in ARSACS HDFs under starvation conditions. These data show that loss of sacsin effects the organization of intermediate filaments in multiple cell types, which impacts the cellular distribution of other organelles and influences autophagic activity., (© The Author 2017. Published by Oxford University Press.)

Published

2017

29. Purkinje neuron Ca2+ influx reduction rescues ataxia in SCA28 model.

Author

Maltecca F, Baseggio E, Consolato F, Mazza D, Podini P, Young SM Jr, Drago I, Bahr BA, Puliti A, Codazzi F, Quattrini A, and Casari G

Subjects

ATP-Dependent Proteases genetics, ATP-Dependent Proteases metabolism, ATPases Associated with Diverse Cellular Activities, Animals, Calcium Signaling, Ceftriaxone pharmacology, Ceftriaxone therapeutic use, Dendrites metabolism, Dendrites pathology, Disease Models, Animal, Drug Evaluation, Preclinical, Humans, Mice, Inbred BALB C, Mice, Transgenic, Mitochondria metabolism, Mitochondria pathology, Psychomotor Performance, Spinocerebellar Ataxias congenital, Spinocerebellar Degenerations drug therapy, Calcium metabolism, Purkinje Cells physiology, Spinocerebellar Degenerations metabolism

Abstract

Spinocerebellar ataxia type 28 (SCA28) is a neurodegenerative disease caused by mutations of the mitochondrial protease AFG3L2. The SCA28 mouse model, which is haploinsufficient for Afg3l2, exhibits a progressive decline in motor function and displays dark degeneration of Purkinje cells (PC-DCD) of mitochondrial origin. Here, we determined that mitochondria in cultured Afg3l2-deficient PCs ineffectively buffer evoked Ca²⁺ peaks, resulting in enhanced cytoplasmic Ca²⁺ concentrations, which subsequently triggers PC-DCD. This Ca²⁺-handling defect is the result of negative synergism between mitochondrial depolarization and altered organelle trafficking to PC dendrites in Afg3l2-mutant cells. In SCA28 mice, partial genetic silencing of the metabotropic glutamate receptor mGluR1 decreased Ca²⁺ influx in PCs and reversed the ataxic phenotype. Moreover, administration of the β-lactam antibiotic ceftriaxone, which promotes synaptic glutamate clearance, thereby reducing Ca²⁺ influx, improved ataxia-associated phenotypes in SCA28 mice when given either prior to or after symptom onset. Together, the results of this study indicate that ineffective mitochondrial Ca²⁺ handling in PCs underlies SCA28 pathogenesis and suggest that strategies that lower glutamate stimulation of PCs should be further explored as a potential treatment for SCA28 patients.

Published

2015

30. Late onset motoneuron disorder caused by mitochondrial Hsp60 chaperone deficiency in mice.

Author

Magnoni R, Palmfeldt J, Christensen JH, Sand M, Maltecca F, Corydon TJ, West M, Casari G, and Bross P

Subjects

Animals, Blotting, Western, Chaperonin 60 genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Mitochondria genetics, Mitochondria pathology, Mitochondrial Proteins genetics, Motor Neuron Disease genetics, Nerve Degeneration genetics, Nerve Degeneration metabolism, Nerve Degeneration pathology, Reverse Transcriptase Polymerase Chain Reaction, Chaperonin 60 deficiency, Disease Models, Animal, Electron Transport Chain Complex Proteins metabolism, Mitochondria metabolism, Mitochondrial Proteins deficiency, Motor Neuron Disease physiopathology

Abstract

Cells rely on efficient protein quality control systems (PQCs) to maintain proper activity of mitochondrial proteins. As part of this system, the mitochondrial chaperone Hsp60 assists folding of matrix proteins and it is an essential protein in all organisms. Mutations in Hspd1, the gene encoding Hsp60, are associated with two human inherited diseases of the nervous system, a dominantly inherited form of spastic paraplegia (SPG13) and an autosomal recessively inherited white matter disorder termed MitCHAP60 disease. Although the connection between mitochondrial failure and neurodegeneration is well known in many neurodegenerative disorders, such as Huntington's disease, Parkinson's disease, and hereditary spastic paraplegia, the molecular basis of the neurodegeneration associated with these diseases is still ill-defined. Here, we investigate mice heterozygous for a knockout allele of the Hspd1 gene encoding Hsp60. Our results demonstrate that Hspd1 haploinsufficiency is sufficient to cause a late onset and slowly progressive deficit in motor functions in mice. We furthermore emphasize the crucial role of the Hsp60 chaperone in mitochondrial function by showing that the motor phenotype is associated with morphological changes of mitochondria, deficient ATP synthesis, and in particular, a defect in the assembly of the respiratory chain complex III in neuronal tissues. In the current study, we propose that our heterozygous Hsp60 mouse model is a valuable model system for the investigation of the link between mitochondrial dysfunction and neurodegeneration., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

31. In vivo detection of oxidized proteins: a practical approach to tissue-derived mitochondria.

Author

Maltecca F and Casari G

Subjects

Animals, Blotting, Western, Electrophoresis, Polyacrylamide Gel, Hydrazones metabolism, Mice, Mutation genetics, Organ Specificity, Oxidation-Reduction, Biochemistry methods, Brain metabolism, Mitochondria metabolism, Mitochondrial Proteins metabolism

Abstract

Mitochondria are the major producers of free radical oxygen species (ROS) as well as the major target of oxidative damage. Defects in the mitochondrial respiratory chain complexes can increase ROS production and reduce ROS removal, leading to oxidative modification of proteins, lipids, and DNA. AAA proteases of the inner mitochondrial membrane, paraplegin and AFG3L2, participate in the biogenesis and maintenance of respiratory chain complexes. These proteins form hetero-oligomeric paraplegin/AFG3L2 and homo-oligomeric AFG3L2 complexes named m-AAA proteases. Inactivation of m-AAA proteases causes respiratory defects and altered mitochondrial morphology both in yeast and in mammals. In fact, mouse models defective for Afg3l2 display a very severe neurological syndrome and die within two weeks after birth. They display widespread morphological alterations of mitochondria in the central and peripheral nervous system and deficiencies in respiratory chain complex I and in complex III, which are major producers of ROS in physiological and especially in pathological conditions. Therefore, an efficient and reliable methodology to monitor the effect of increased ROS production is useful for accurately phenotyping cellular and animal models mutants in m-AAA. By measuring carbonyl formation as marker of protein oxidation, we have shown that respiratory defects cause oxidative damage in Afg3l2 mutants, indicating that oxidative stress is crucial in the pathogenesis of m-AAA deficiency.

Published

2010

32. Haploinsufficiency of AFG3L2, the gene responsible for spinocerebellar ataxia type 28, causes mitochondria-mediated Purkinje cell dark degeneration.

Author

Maltecca F, Magnoni R, Cerri F, Cox GA, Quattrini A, and Casari G

Subjects

ATP-Dependent Proteases, ATPases Associated with Diverse Cellular Activities, Adenosine Triphosphatases genetics, Adenosine Triphosphate metabolism, Aging, Animals, Apoptosis physiology, Cerebellum pathology, Cerebellum physiopathology, Disease Models, Animal, Ganglia, Spinal cytology, Ganglia, Spinal metabolism, Ganglia, Spinal pathology, Gliosis pathology, Gliosis physiopathology, Mice, Mice, Mutant Strains, Mitochondria pathology, Motor Activity genetics, Motor Activity physiology, Motor Neurons cytology, Motor Neurons metabolism, Nerve Degeneration pathology, Purkinje Cells pathology, Reactive Oxygen Species metabolism, Spinal Cord cytology, Spinal Cord metabolism, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias pathology, Adenosine Triphosphatases metabolism, Mitochondria physiology, Nerve Degeneration physiopathology, Purkinje Cells physiology, Spinocerebellar Ataxias physiopathology

Abstract

Paraplegin and AFG3L2 are ubiquitous nuclear-encoded mitochondrial proteins that form hetero-oligomeric paraplegin-AFG3L2 and homo-oligomeric AFG3L2 complexes in the inner mitochondrial membrane, named m-AAA proteases. These complexes ensure protein quality control in the inner membrane, jointly with a chaperone-like activity on the respiratory chain complexes. Despite coassembling in the same complex, mutations of either paraplegin or AFG3L2 cause two different neurodegenerative disorders. Indeed, mutations of paraplegin are responsible for a recessive form of hereditary spastic paraplegia, whereas mutations of AFG3L2 have been recently associated to a dominant form of spinocerebellar ataxia (SCA28). In this work, we report that the mouse model haploinsufficient for Afg3l2 recapitulates important pathophysiological features of the human disease, thus representing the first SCA28 model. Furthermore, we propose a pathogenetic mechanism in which respiratory chain dysfunction and increased reactive oxygen species production caused by Afg3l2 haploinsufficiency lead to dark degeneration of Purkinje cells and cerebellar dysfunction.

Published

2009

33. The mitochondrial protease AFG3L2 is essential for axonal development.

Author

Maltecca F, Aghaie A, Schroeder DG, Cassina L, Taylor BA, Phillips SJ, Malaguti M, Previtali S, Guénet JL, Quattrini A, Cox GA, and Casari G

Subjects

ATP-Dependent Proteases, ATPases Associated with Diverse Cellular Activities, Adenosine Triphosphatases genetics, Amino Acid Sequence, Animals, Animals, Newborn, Axons pathology, Axons physiology, Mice, Mice, Mutant Strains, Mitochondria genetics, Mitochondria pathology, Mitochondrial Proteins genetics, Molecular Sequence Data, Adenosine Triphosphatases biosynthesis, Axons enzymology, Mitochondria enzymology, Mitochondrial Proteins biosynthesis

Abstract

The mitochondrial metalloprotease AFG3L2 assembles with the homologous protein paraplegin to form a supracomplex in charge of the essential protein quality control within mitochondria. Mutations of paraplegin cause a specific axonal degeneration of the upper motoneuron and, therefore, hereditary spastic paraplegia. Here we present two Afg3l2 murine models: a newly developed null and a spontaneous mutant that we found carrier of a missense mutation. Contrasting with the mild and late onset axonal degeneration of paraplegin-deficient mouse, Afg3l2 models display a marked impairment of axonal development with delayed myelination and poor axonal radial growth leading to lethality at P16. The increased severity of the Afg3l2 mutants is explained by two main molecular features that differentiate AFG3L2 from paraplegin: its higher neuronal expression and its versatile ability to support both hetero-oligomerization and homo-oligomerization. Our data assign to AFG3L2 a crucial role by linking mitochondrial metabolism and axonal development. Moreover, we propose AFG3L2 as an excellent candidate for motoneuron and cerebellar diseases with early onset unknown etiology.

Published

2008

34. Behavioral disorder, dementia, ataxia, and rigidity in a large family with TATA box-binding protein mutation.

Author

Bruni AC, Takahashi-Fujigasaki J, Maltecca F, Foncin JF, Servadio A, Casari G, D'Adamo P, Maletta R, Curcio SA, De Michele G, Filla A, El Hachimi KH, and Duyckaerts C

Subjects

Adult, Aged, Behavioral Symptoms genetics, Behavioral Symptoms pathology, Behavioral Symptoms psychology, Brain pathology, Dementia pathology, Dementia psychology, Female, Humans, Male, Middle Aged, Muscle Rigidity pathology, Muscle Rigidity psychology, Pedigree, Spinocerebellar Ataxias pathology, Spinocerebellar Ataxias psychology, Dementia genetics, Muscle Rigidity genetics, Mutation, Spinocerebellar Ataxias genetics, TATA-Box Binding Protein genetics

Abstract

Background: Spinocerebellar ataxia type 17 is an autosomal dominant cerebellar ataxia caused by a CAG repeat expansion in the TATA box-binding protein gene. Ataxia is typically the first sign whereas behavioral symptoms occur later., Objective: To characterize the unusual phenotypic expression of a large spinocerebellar ataxia type 17 kindred., Design: Clinical, neuropathological, and molecular genetic characterization of a 4-generation family with 16 affected patients., Results: Behavioral symptoms and frontal impairment dominated the early stages preceding ataxia, rigidity, and dystonic movements. Neuropathological examination showed cortical, subcortical, and cerebellar atrophy. Purkinje cell loss and gliosis, pseudohypertrophic degeneration of the inferior olive, marked neuronal loss and gliosis in the caudate nucleus, and in the medial thalamic nuclei were salient features together with neuronal intranuclear inclusions stained with anti-TATA box-binding protein and antipolyglutamine antibodies. The disease was caused by a stable 52 CAG repeat expansion of the TATA box-binding protein gene, although there was apparent variability in the age of onset., Conclusion: The characteristics of this family broaden the clinical picture of spinocerebellar ataxia type 17: initial presenile dementia with behavioral symptoms should be added to ataxia, rigidity, and dystonic movements, which are more commonly encountered.

Published

2004

35. [Modified Hanau technic. Setting up of teeth. Modified occlusal systematization (by the Lauritzen technic). 3].

Author

Maltecca F, Spirgi M, Berta JJ, Pouezat JR, Chevrolet S, and Metral J

Subjects

Dental Occlusion, Denture, Complete, Tooth, Artificial

Published

1971