Your search keyword '"Dominant Optic Atrophy"' showing total 23 results

1. OPA1 Dominant Optic Atrophy: Diagnostic Approach in the Pediatric Population

Author

Natalia Arruti, Patricia Rodríguez-Solana, María Nieves-Moreno, Marta Guerrero-Carretero, Ángela del Pozo, Victoria E. F. Montaño, Fernando Santos-Simarro, Emi Rikeros-Orozco, Luna Delgado-Mora, Elena Vallespín, and Susana Noval

Subjects

Microbiology (medical), General Medicine, Molecular Biology, Microbiology, dominant optic atrophy, Kjer type, OPA1, mitochondrial neuropathies

Abstract

A clinical and genetic study was conducted with pediatric patients and their relatives with optic atrophy 1 (OPA1) mutations to establish whether there is a genotype–phenotype correlation among the variants detected within and between families. Eleven children with a confirmed OPA1 mutation were identified during the study period. The main initial complaint was reduced visual acuity (VA), present in eight patients of the cohort. Eight of eleven patients had a positive family history of optic atrophy. The mean visual acuity at the start of the study was 0.40 and 0.44 LogMAR in the right and left eye, respectively. At the end of the study, the mean visual acuity was unchanged. Optical coherence tomography during the first visit showed a mean retinal nerve fiber layer thickness of 81.6 microns and 80.5 microns in the right and left eye, respectively; a mean ganglion cell layer of 52.5 and 52.4 microns, respectively, and a mean central macular thickness of 229.5 and 233.5 microns, respectively. The most common visual field defect was a centrocecal scotoma, and nine out of eleven patients showed bilateral temporal disc pallor at baseline. Sequencing of OPA1 showed seven different mutations in the eleven patients, one of which, NM_130837.3: c.1406_1407del (p.Thr469LysfsTer16), has not been previously reported. Early diagnosis of dominant optic atrophy is crucial, both for avoiding unnecessary consultations and/or treatments and for appropriate genetic counseling.

Published

2023

2. Autosomal dominant optic atrophy: A novel treatment for OPA1 splice defects using U1 snRNA adaption

Author

Bernd Wissinger, Christoph Jüschke, Thomas Klopstock, Marta Owczarek-Lipska, John Neidhardt, Claudia B. Catarino, and Faculteit Medische Wetenschappen/UMCG

Subjects

EXPRESSION, endocrine system, ExSpeU1, U1 snRNA, ISOFORMS, DOA, RM1-950, Biology, GENE THERAPEUTIC APPROACH, medicine.disease_cause, OPA1, DISEASE, ADOA, splicing, Exon, Drug Discovery, Optic Atrophy Type 1, medicine, splice, STRATEGY, ddc:610, Dominant Optic Atrophy, MUTATION, Gene, Genetics, SPECTRUM, Mutation, Intron, SMALL NUCLEAR-RNA, medicine.disease, CORRECT, gene therapy, eye diseases, LONG, RNA splicing, Molecular Medicine, Optic Atrophy 1, Therapeutics. Pharmacology, Haploinsufficiency, Autosomal Dominant Optic Atrophy

Abstract

Autosomal dominant optic atrophy (ADOA) is frequently caused by mutations in the optic atrophy 1 (OPA1) gene, with haploinsufficiency being the major genetic pathomechanism. Almost 30% of the OPA1-associated cases suffer from splice defects. We identified a novel OPA1 mutation, c.1065+5G>A, in patients with ADOA. In patient-derived fibroblasts, the mutation led to skipping of OPA1 exon 10, reducing the OPA1 protein expression by approximately 50%. We developed a molecular treatment to correct the splice defect in OPA1 using engineered U1 splice factors retargeted to different locations in OPA1 exon 10 or intron 10. The strongest therapeutic effect was detected when U1 binding was engineered to bind to intron 10 at position +18, a position predicted by bioinformatics to be a promising binding site. We were able to significantly silence the effect of the mutation (skipping of exon 10) and simultaneously increase the expression level of normal transcripts. Retargeting U1 to the canonical splice donor site did not lead to a detectable splice correction. This proof-of-concept study indicates for the first time the feasibility of splice mutation correction as a treatment option for ADOA. Increasing the amount of correctly spliced OPA1 transcripts may suffice to overcome the haploinsufficiency.

Published

2021

3. Next-Generation Sequencing Identifies Novel PMPCA Variants in Patients with Late-Onset Dominant Optic Atrophy

Author

Majida Charif, Arnaud Chevrollier, Naïg Gueguen, Selma Kane, Céline Bris, David Goudenège, Valerie Desquiret-Dumas, Isabelle Meunier, Fanny Mochel, Luc Jeanjean, Fanny Varenne, Vincent Procaccio, Pascal Reynier, Dominique Bonneau, Patrizia Amati-Bonneau, and Guy Lenaers

Subjects

Genetics, dominant optic atrophy, mitochondrial peptidase, mitochondrial dynamic, heterozygous variants, retinal ganglion cell degeneration, Genetics (clinical)

Abstract

Dominant Optic Atrophy (DOA) is one of the most common inherited mitochondrial diseases, leading to blindness. It is caused by the chronic degeneration of the retinal ganglion cells (RGCs) and their axons forming the optic nerve. Until now, DOA has been mainly associated with genes encoding proteins involved in mitochondrial network dynamics. Using next-generation and exome sequencing, we identified for the first time heterozygous PMPCA variants having a causative role in the pathology of late-onset primary DOA in five patients. PMPCA encodes an α subunit of the mitochondrial peptidase (MPP), responsible for the cleavage and maturation of the mitochondrial precursor proteins imported from the cytoplasm into mitochondria. Recently, PMPCA has been identified as the gene responsible for Autosomal Recessive Cerebellar Ataxia type 2 (SCAR2) and another severe recessive mitochondrial disease. In this study, four PMPCA variants were identified, two are frameshifts (c.309delA and c.820delG) classified as pathogenic and two are missenses (c.1363G>A and c.1547G>A) classified with uncertain pathological significance. Functional assays on patients’ fibroblasts show a hyperconnection of the mitochondrial network and revealed that frameshift variants reduced α-MPP levels, while not significantly affecting the respiratory machinery. These results suggest that alterations in mitochondrial peptidase function can affect the fusion-fission balance, a key element in maintaining the physiology of retinal ganglion cells, and consequently lead to their progressive degeneration.

Published

2022

4. Autosomal dominant optic atrophy: A novel treatment for

Author

Christoph, Jüschke, Thomas, Klopstock, Claudia B, Catarino, Marta, Owczarek-Lipska, Bernd, Wissinger, and John, Neidhardt

Subjects

endocrine system, splicing, ExSpeU1, U1 snRNA, Optic Atrophy Type 1, Original Article, DOA, Dominant Optic Atrophy, gene therapy, OPA1, eye diseases, ADOA, Autosomal Dominant Optic Atrophy

Abstract

Autosomal dominant optic atrophy (ADOA) is frequently caused by mutations in the optic atrophy 1 (OPA1) gene, with haploinsufficiency being the major genetic pathomechanism. Almost 30% of the OPA1-associated cases suffer from splice defects. We identified a novel OPA1 mutation, c.1065+5G>A, in patients with ADOA. In patient-derived fibroblasts, the mutation led to skipping of OPA1 exon 10, reducing the OPA1 protein expression by approximately 50%. We developed a molecular treatment to correct the splice defect in OPA1 using engineered U1 splice factors retargeted to different locations in OPA1 exon 10 or intron 10. The strongest therapeutic effect was detected when U1 binding was engineered to bind to intron 10 at position +18, a position predicted by bioinformatics to be a promising binding site. We were able to significantly silence the effect of the mutation (skipping of exon 10) and simultaneously increase the expression level of normal transcripts. Retargeting U1 to the canonical splice donor site did not lead to a detectable splice correction. This proof-of-concept study indicates for the first time the feasibility of splice mutation correction as a treatment option for ADOA. Increasing the amount of correctly spliced OPA1 transcripts may suffice to overcome the haploinsufficiency., Graphical abstract, Optic atrophy is one of the most common inherited optic neuropathies, with progressive loss of vision starting in childhood. In patient-derived fibroblasts, the authors identified a mutation in OPA1 causing aberrant precursor mRNA splicing concomitant with reduced protein expression. Using engineered small nuclear RNAs, they could partially restore normal splicing.

Published

2020

5. Optimized OPA1 Isoforms 1 and 7 Provide Therapeutic Benefit in Models of Mitochondrial Dysfunction

Author

Daniel M. Maloney, Naomi Chadderton, Sophia Millington-Ward, Arpad Palfi, Ciara Shortall, James J. O’Byrne, Lorraine Cassidy, David Keegan, Peter Humphries, Paul Kenna, and Gwyneth Jane Farrar

Subjects

Gene isoform, endocrine system, Mitochondrion, Biology, bioenergetics, lcsh:RC321-571, Optic neuropathy, Atrophy, medicine, dominant optic atrophy, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, optic atrophy 1, Original Research, General Neuroscience, AAV, medicine.disease, gene therapy, eye diseases, optic neuropathy, Cell biology, mitochondria, medicine.anatomical_structure, retinal ganglion cells, Retinal ganglion cell, Knockout mouse, Optic nerve, Optic Atrophy 1, Neuroscience

Abstract

Optic Atrophy 1 (OPA1) is a mitochondrially targeted GTPase that plays a pivotal role in mitochondrial health, with mutations causing severe mitochondrial dysfunction and typically associated with Dominant Optic Atrophy (DOA), a progressive blinding disease involving retinal ganglion cell loss and optic nerve damage. In the current study, we investigate the use of codon-optimized versions of OPA1 isoform 1 and 7 as potential therapeutic interventions in a range of in vitro and in vivo models of mitochondrial dysfunction. We demonstrate that both isoforms perform equally well in ameliorating mitochondrial dysfunction in OPA1 knockout mouse embryonic fibroblast cells but that OPA1 expression levels require tight regulation for optimal benefit. Of note, we demonstrate for the first time that both OPA1 isoform 1 and 7 can be used independently to protect spatial visual function in a murine model of retinal ganglion cell degeneration caused by mitochondrial dysfunction, as well as providing benefit to mitochondrial bioenergetics in DOA patient derived fibroblast cells. These results highlight the potential value of OPA1-based gene therapy interventions.

Published

2020

6. Neuro-ophthalmic manifestations of mitochondrial disorders and their management

Author

Neha K Irani, Nancy J. Newman, and Jane H. Lock

Subjects

0301 basic medicine, medicine.medical_specialty, Dominant optic atrophy, genetic structures, Mitochondrial disease, Review Article, Extraocular muscles, Optic neuropathy, 03 medical and health sciences, 0302 clinical medicine, lcsh:Ophthalmology, medicine, pigmentary retinopathy, macular pattern dystrophy, Retinal pigment epithelium, business.industry, External ophthalmoplegia, Pigmentary Retinopathy, medicine.disease, Dermatology, progressive external ophthalmoplegia, eye diseases, Ophthalmology, mitochondrial disease, 030104 developmental biology, medicine.anatomical_structure, lcsh:RE1-994, Lactic acidosis, 030221 ophthalmology & optometry, Optic nerve, sense organs, business, Leber hereditary optic neuropathy

Abstract

The visual system has high metabolic requirements and is therefore particularly vulnerable to mitochondrial dysfunction. The most commonly affected tissues include the extraocular muscles, photoreceptors, retinal pigment epithelium, optic nerve and visual cortex. Hence, the most common manifestations of mitochondrial disorders are progressive external ophthalmoplegia, macular pattern dystrophy, pigmentary retinopathy, optic neuropathy and retrochiasmal visual field loss. With the exception of Leber hereditary optic neuropathy and stroke-like episodes seen in mitochondrial encephalopathy, lactic acidosis and stroke-like episodes, the majority of neuro-ophthalmic manifestations have an insidious onset. As such, some patients may not recognize subtle progressive visual symptoms. When mitochondrial disorders are highly suspected, meticulous examination performed by an ophthalmologist with targeted ancillary testing can help confirm the diagnosis. Similarly, neuro-ophthalmic symptoms and signs may be the first indication of mitochondrial disease and should prompt systemic investigations for potentially life-threatening associations, such as cardiac conduction defects. Finally, the ophthalmologist can offer symptomatic treatments for some of the most disabling manifestations of these disorders.

Published

2020

7. Dominant optic atrophy: Culprit mitochondria in the optic nerve

Author

Christoph Jüschke, Pascal Reynier, Guy Lenaers, Yannick Le Dantec, Sarah Decembrini, Sebastian Swirski, Sinja Kieninger, Ungsoo Samuel Kim, Cavit Agca, Bernd Wissinger, Ting Xiao, Albert Neutzner, John Neidhardt, Patrick Yu-Wai-Man, MitoVasc - Physiopathologie Cardiovasculaire et Mitochondriale (MITOVASC), Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), University of Basel (Unibas), University Hospital Basel [Basel], University of Oldenburg, University of Tübingen, Sabanci University [Istanbul], University of Cambridge [UK] (CAM), Cambridge University Hospitals - NHS (CUH), Centre Hospitalier Universitaire d'Angers (CHU Angers), PRES Université Nantes Angers Le Mans (UNAM), University College of London [London] (UCL), and LENAERS, Guy

Subjects

Retinal Ganglion Cells, Mitochondrial DNA, Dominant optic atrophy, genetic structures, [SDV]Life Sciences [q-bio], Mitochondrial disease, Mitochondrion, Biology, OPA1, Retinal ganglion, GTP Phosphohydrolases, Mice, Atrophy, Optic Atrophy, Autosomal Dominant, medicine, Animals, Humans, Retina, Optic Nerve, medicine.disease, eye diseases, Sensory Systems, Mitochondria, [SDV] Life Sciences [q-bio], Ophthalmology, medicine.anatomical_structure, Optic nerve, Intermembrane space, Neuroscience

Abstract

International audience; Dominant optic atrophy (DOA) is an inherited mitochondrial disease leading to specific degeneration of retinal ganglion cells (RGCs), thus compromising transmission of visual information from the retina to the brain. Usually, DOA starts during childhood and evolves to poor vision or legal blindness, affecting the central vision, whilst sparing the peripheral visual field. In 20% of cases, DOA presents as syndromic disorder, with secondary symptoms affecting neuronal and muscular functions. Twenty years ago, we demonstrated that heterozygous mutations in OPA1 are the most frequent molecular cause of DOA. Since then, variants in additional genes, whose functions in many instances converge with those of OPA1, have been identified by next generation sequencing. OPA1 encodes a dynamin-related GTPase imported into mitochondria and located to the inner membrane and intermembrane space. The many OPA1 isoforms, resulting from alternative splicing of three exons, form complex homopolymers that structure mitochondrial cristae, and contribute to fusion of the outer membrane, thus shaping the whole mitochondrial network. Moreover, OPA1 is required for oxidative phosphorylation, maintenance of mitochondrial genome, calcium homeostasis and regulation of apoptosis, thus making OPA1 the Swiss army-knife of mitochondria. Understanding DOA pathophysiology requires the understanding of RGC peculiarities with respect to OPA1 functions. Besides the tremendous energy requirements of RGCs to relay visual information from the eye to the brain, these neurons present unique features related to their differential environments in the retina, and to the anatomical transition occurring at the lamina cribrosa, which parallel major adaptations of mitochondrial physiology and shape, in the pre- and post-laminar segments of the optic nerve. Three DOA mouse models, with different Opa1 mutations, have been generated to study intrinsic mechanisms responsible for RGC degeneration, and these have further revealed secondary symptoms related to mitochondrial dysfunctions, mirroring the more severe syndromic phenotypes seen in a subgroup of patients. Metabolomics analyses of cells, mouse organs and patient plasma mutated for OPA1 revealed new unexpected pathophysiological mechanisms related to mitochondrial dysfunction, and biomarkers correlated quantitatively to the severity of the disease. Here, we review and synthesize these data, and propose different approaches for embracing possible therapies to fulfil the unmet clinical needs of this disease, and provide hope to affected DOA patients.

Published

2020

8. OPA1: How much do we know to approach therapy?

Author

Claudia Zanna, Michela Rugolo, Mario Fogazza, Valentina Del Dotto, Guy Lenaers, Valerio Carelli, Physiopathologie Cardiovasculaire et Mitochondriale (MITOVASC), Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Del Dotto, Valentina, Fogazza, Mario, Lenaers, Guy, Rugolo, Michela, Carelli, Valerio, and Zanna, Claudia

Subjects

0301 basic medicine, endocrine system, Mitochondrial DNA, DOA therapy, GTPase, Biology, DNA, Mitochondrial, Mitochondrial Dynamics, GTP Phosphohydrolases, 03 medical and health sciences, Atrophy, Optic Atrophy, Autosomal Dominant, medicine, Animals, Humans, dominant optic atrophy, [SDV.MHEP.OS]Life Sciences [q-bio]/Human health and pathology/Sensory Organs, Pharmacology, Cellular pathways, Mitochondria dynamics, medicine.disease, Phenotype, eye diseases, Mitochondria, 3. Good health, 030104 developmental biology, Mutation, OPA1 mutation, OPA1 mutations, Neuroscience

Abstract

International audience; OPA1 is a GTPase that controls several functions, such as mitochondrial dynamics and energetics, mtDNA maintenance and cristae integrity. In the last years, there have been described other cellular pathways and mechanisms involving OPA1 directly or through its interaction. All this new information, by implementing our knowledge on OPA1 is instrumental to elucidating the pathogenic mechanisms of OPA1 mutations. Indeed, these are associated with dominant optic atrophy (DOA), one of the most common inherited optic neuropathies, and with an increasing number of heterogeneous neurodegenerative disorders. In this review, we overview all recent findings on OPA1 protein functions, on its dysfunction and related clinical phenotypes, focusing on the current therapeutic options and future perspectives to treat DOA and the other associated neurological disorders due to OPA1 mutations.

Published

2018

9. Incomplete penetrance in mitochondrial optic neuropathies

Author

Francesca Tagliavini, Valentina Del Dotto, Leonardo Caporali, Mariantonietta Capristo, Valerio Carelli, Chiara La Morgia, Alessandra Maresca, Maria Lucia Valentino, Caporali, Leonardo, Maresca, Alessandra, Capristo, Mariantonietta, DEL DOTTO, Valentina, Tagliavini, Francesca, Valentino, MARIA LUCIA, LA MORGIA, Chiara, and Carelli, Valerio

Subjects

0301 basic medicine, Mitochondrial DNA, Dominant optic atrophy, genetic structures, Penetrance, Optic Atrophy, Hereditary, Leber, Biology, DNA, Mitochondrial, Genetic modifier, Optic neuropathy, 03 medical and health sciences, 0302 clinical medicine, Optic Atrophy, Autosomal Dominant, Optic Nerve Diseases, medicine, Humans, Molecular Biology, Incomplete penetrance, Genetics, Mechanism (biology), Leber's hereditary optic neuropathy, Environmental Exposure, Cell Biology, medicine.disease, eye diseases, Mitochondria, 030104 developmental biology, Mitochondrial biogenesis, Molecular Medicine, Environmental trigger, Mitochondrial optic neuropathies, Inherited optic neuropathie, 030217 neurology & neurosurgery, Leber's Hereditary Optic Neuropathy, Human mitochondrial DNA haplogroup

Abstract

Incomplete penetrance characterizes the two most frequent inherited optic neuropathies, Leber's Hereditary Optic Neuropathy (LHON) and dominant optic atrophy (DOA), due to genetic errors in the mitochondrial DNA (mtDNA) and the nuclear DNA (nDNA), respectively. For LHON, compelling evidence has accumulated on the complex interplay of mtDNA haplogroups and environmental interacting factors, whereas the nDNA remains essentially non informative. However, a compensatory mechanism of activated mitochondrial biogenesis and increased mtDNA copy number, possibly driven by a permissive nDNA background, is documented in LHON; when successful it maintains unaffected the mutation carriers, but in some individuals it might be hampered by tobacco smoking or other environmental factors, resulting in disease onset. In females, mitochondrial biogenesis is promoted and maintained within the compensatory range by estrogens, partially explaining the gender bias in LHON. Concerning DOA, none of the above mechanisms has been fully explored, thus mtDNA haplogroups, environmental factors such as tobacco and alcohol, and further nDNA variants may all participate as protective factors or, on the contrary, favor disease expression and severity. Next generation sequencing, complemented by transcriptomics and proteomics, may provide some answers in the next future, even if the multifactorial model that seems to apply to incomplete penetrance in mitochondrial optic neuropathies remains problematic, and careful stratification of patients will play a key role for data interpretation. The deep understanding of which factors impinge on incomplete penetrance may shed light on the pathogenic mechanisms leading to optic nerve atrophy, on their possible compensation and, thus, on development of therapeutic strategies.

Published

2017

10. The Influence of Mitochondrial Dynamics and Function on Retinal Ganglion Cell Susceptibility in Optic Nerve Disease

Author

Nicole A. Muench, Robert W. Nickells, Ryan J. Donahue, Margaret E. Maes, Sonia Patel, and Akihiro Ikeda

Subjects

Retinal Ganglion Cells, Cell type, genetic structures, QH301-705.5, Review, Biology, Mitochondrion, Mitochondrial Dynamics, Retinal ganglion, optic nerve, Optic neuropathy, Optic Nerve Diseases, medicine, Animals, Humans, Molecular Targeted Therapy, dominant optic atrophy, Biology (General), Neurodegeneration, neurodegeneration, General Medicine, medicine.disease, eye diseases, mitochondria, glaucoma, medicine.anatomical_structure, Retinal ganglion cell, Optic nerve, Axoplasmic transport, sense organs, Energy Metabolism, metabolism, Neuroscience

Abstract

The important roles of mitochondrial function and dysfunction in the process of neurodegeneration are widely acknowledged. Retinal ganglion cells (RGCs) appear to be a highly vulnerable neuronal cell type in the central nervous system with respect to mitochondrial dysfunction but the actual reasons for this are still incompletely understood. These cells have a unique circumstance where unmyelinated axons must bend nearly 90° to exit the eye and then cross a translaminar pressure gradient before becoming myelinated in the optic nerve. This region, the optic nerve head, contains some of the highest density of mitochondria present in these cells. Glaucoma represents a perfect storm of events occurring at this location, with a combination of changes in the translaminar pressure gradient and reassignment of the metabolic support functions of supporting glia, which appears to apply increased metabolic stress to the RGC axons leading to a failure of axonal transport mechanisms. However, RGCs themselves are also extremely sensitive to genetic mutations, particularly in genes affecting mitochondrial dynamics and mitochondrial clearance. These mutations, which systemically affect the mitochondria in every cell, often lead to an optic neuropathy as the sole pathologic defect in affected patients. This review summarizes knowledge of mitochondrial structure and function, the known energy demands of neurons in general, and places these in the context of normal and pathological characteristics of mitochondria attributed to RGCs.

Published

2021

11. A randomized, placebo-controlled trial of the benzoquinone idebenone in a mouse model of OPA1-related dominant optic atrophy reveals a limited therapeutic effect on retinal ganglion cell dendropathy and visual function

Author

Smith, T.G., Seto, S., Ganne, P., and Votruba, M.

Subjects

mitochondria, idebenone, genetic structures, Neuroscience(all), NQO1, RE, sense organs, dominant optic atrophy, retinal ganglion cell, OPA1, eye diseases

Abstract

Dominant optic atrophy (DOA) arises from mutations in the OPA1 gene that promotes fusion of the inner mitochondrial membrane and plays a role in maintaining ATP levels. Patients display optic disc pallor, retinal ganglion cell (RGC) loss and bilaterally reduced vision. We report a randomized, placebo-controlled trial of idebenone at 2000 mg/kg/day in 56 Opa1 mutant mice (B6;C3-Opa1Q285STOP), with RGC dendropathy and visual loss, and 63 wildtype mice. We assessed cellular responses in the retina, brain and liver and RGC morphology, by diolistic labeling, Sholl analysis and quantification of dendritic morphometric features. Vision was assessed by optokinetic responses. ATP levels were raised by 0.57 nmol/mg (97.73%, p = 0.035) in brain from idebenone-treated Opa1 mutant mice, but in the liver there was an 80.35% (p = 0.011) increase in oxidative damage. NQO1 expression in Opa1 mutant mice was reduced in the brain (to 30.5%, p = 0.002) but not in retina, and neither expression level was induced by idebenone. ON-center RGCs failed to show major recovery, other than improvements in secondary dendritic length (by 53.89%, p = 0.052) and dendritic territory (by 2.22 × 104 μm2 or 90.24%, p = 0.074). An improvement in optokinetic response was observed (by 12.2 ± 3.2 s, p = 0.003), but this effect was not sustained over time. OFF-center RGCs from idebenone-treated wildtype mice showed shrinkage in total dendritic length by 2.40 mm (48.05%, p = 0.025) and a 47.37% diminished Sholl profile (p = 0.029). Visual function in wildtype idebenone-treated mice was impaired (2.9 fewer head turns than placebo, p = 0.007). Idebenone appears largely ineffective in protecting Opa1 heterozygous RGCs from dendropathy. The detrimental effect of idebenone in wildtype mice has not been previously observed and raises some concerns.

Published

2016

12. Mutations in SLC25A46, encoding a UGO1-like protein, cause an optic atrophy spectrum disorder

Author

Antonio Barrientos, Kristen L. Sund, Julia E. Dallman, Adriana P. Rebelo, Stephan Züchner, Zubair M. Ahmed, Xinjian Wang, Claudia Zanna, Andrea H. Németh, Leonardo Caporali, Carlos E. Prada, Neville Patel, Ion J. Campeanu, Feifei Tao, Susan M. Downes, Laura Krueger, Alessandra Maresca, Cynthia A. Prows, Anthony Antonellis, Saskia Groenewald, Lisa Abreu, Fiorella Speziani, Alleene V. Strickland, Yaping Yang, Michael A. Gonzalez, Taosheng Huang, Elizabeth K. Schorry, Valerio Carelli, Chiara La Morgia, Rebecca Schüle, Flavia Fontanesi, Laurie B. Griffin, Alexander J. Abrams, Robert B. Hufnagel, Jeffery Prince, Rocco Liguori, Raffaele Lodi, Omar A. Abdul-Rahman, Holly H. Zimmerman, Yanyan Peng, Abrams, A.J., Hufnagel, R.B., Rebelo, A., Zanna, C., Patel, N., Gonzalez, M.A., Campeanu, I.J., Griffin, L.B., Groenewald, S., Strickland, A.V., Tao, F., Speziani, F., Abreu, L., Schule, R., Caporali, L., La Morgia, C., Maresca, A., Liguori, R., Lodi, R., Ahmed, Z.M., Sund, K.L., Wang, X., Krueger, L.A., Peng, Y., Prada, C.E., Prows, C.A., Schorry, E.K., Antonellis, A., Zimmerman, H.H., Abdul-Rahman, O.A., Yang, Y., Downes, S.M., Prince, J., Fontanesi, F., Barrientos, A., Nemeth, A.H., Carelli, V., Huang, T., Zuchner, S., and Dallman, J.E.

Subjects

Male, Embryo, Nonmammalian, MFN2, Muscle Proteins, IMMT protein, human, DOA, genetics [Muscle Proteins], medicine.disease_cause, Animals, Genetically Modified, pathology [Optic Atrophy, Autosomal Dominant], metabolism [Optic Atrophy, Autosomal Dominant], 0302 clinical medicine, Charcot-Marie-Tooth Disease, Chlorocebus aethiops, genetics [Phosphate Transport Proteins], genetics [Exome], Phosphate Transport Proteins, Exome, metabolism [Zebrafish], genetics [Genetic Predisposition to Disease], embryology [Embryo, Nonmammalian], Zebrafish, Genetics, 0303 health sciences, Mutation, Microscopy, Confocal, biology, Pedigree, genetics [Membrane Proteins], xonal peripheral neuropathy, mitochondrial fusion, Mitochondrial Membranes, COS Cells, Female, genetics [Mitochondrial Proteins], RNA Interference, genetics [Charcot-Marie-Tooth Disease], Protein Binding, UGO1 protein, S cerevisiae, metabolism [Embryo, Nonmammalian], Saccharomyces cerevisiae Proteins, Dominant optic atrophy, Charcot-Marie-Tooth type 2, CMT2, metabolism [Muscle Proteins], genetics [Optic Atrophy, Autosomal Dominant], metabolism [Phosphate Transport Proteins], Article, ultrastructure [Embryo, Nonmammalian], metabolism [Mitochondrial Proteins], Mitochondrial Proteins, 03 medical and health sciences, Atrophy, Microscopy, Electron, Transmission, ddc:570, Optic Atrophy, Autosomal Dominant, metabolism [Mitochondrial Membranes], medicine, Animals, Humans, Inner membrane, Genetic Predisposition to Disease, Hereditary Neurodegenerative Disorder, genetics [Saccharomyces cerevisiae Proteins], 030304 developmental biology, Membrane Proteins, Sequence Analysis, DNA, metabolism [Saccharomyces cerevisiae Proteins], biology.organism_classification, medicine.disease, eye diseases, HEK293 Cells, metabolism [Charcot-Marie-Tooth Disease], Membrane protein, embryology [Zebrafish], hereditary neurodegenerative disorder, metabolism [Membrane Proteins], 030217 neurology & neurosurgery, SLC25A46 protein, human

Abstract

Dominant optic atrophy (DOA) and axonal peripheral neuropathy (Charcot-Marie-Tooth type 2, or CMT2) are hereditary neurodegenerative disorders most commonly caused by mutations in the canonical mitochondrial fusion genes OPA1 and MFN2, respectively. In yeast, homologs of OPA1 (Mgm1) and MFN2 (Fzo1) work in concert with Ugo1, for which no human equivalent has been identified thus far. By whole-exome sequencing of patients with optic atrophy and CMT2, we identified four families with recessive mutations in SLC25A46. We demonstrate that SLC25A46, like Ugo1, is a modified carrier protein that has been recruited to the outer mitochondrial membrane and interacts with the inner membrane remodeling protein mitofilin (Fcj1). Loss of function in cultured cells and in zebrafish unexpectedly leads to increased mitochondrial connectivity, while severely affecting the development and maintenance of neurons in the fish. The discovery of SLC25A46 strengthens the genetic overlap between optic atrophy and CMT2 while exemplifying a new class of modified solute transporters linked to mitochondrial dynamics.

Published

2015

13. The dynamin GTPase OPA1: More than mitochondria?

Author

Pascale Belenguer and Luca Pellegrini

Subjects

Dynamins, endocrine system, Dominant optic atrophy, Lipolysis, Translocase of the outer membrane, Apoptosis, Biology, OPA1, Mitochondrial Dynamics, Models, Biological, Gene Expression Regulation, Enzymologic, GTP Phosphohydrolases, 03 medical and health sciences, 0302 clinical medicine, Yeasts, Mitochondrial inner membrane fusion, medicine, Animals, Humans, Membrane dynamics, Inner mitochondrial membrane, Molecular Biology, 030304 developmental biology, 0303 health sciences, mtDNA, Cell Biology, medicine.disease, Mitochondrial carrier, eye diseases, Mitochondria, Cell biology, mitochondrial fusion, Translocase of the inner membrane, Optic Atrophy 1, Mitochondrial fission, 030217 neurology & neurosurgery

Abstract

The studies addressing the molecular mechanisms governing mitochondrial fusion and fission have brought to light a small group of dynamin-like GTPases (Guanosine-Triphosphate hydrolase) as central regulators of mitochondrial morphology and cristae remodeling, apoptosis, calcium signaling, and metabolism. One of them is the mammalian OPA1 (Optic atrophy 1) protein, which resides inside the mitochondrion anchored to the inner membrane and, in a cleaved form, is associated to oligomeric complexes, in the intermembrane space of the organelle. Here, we review the studies that have made OPA1 emerge as the best understood regulator of mitochondrial inner membrane fusion and cristae remodeling. Further, we re-examine the findings behind the recent claim that OPA1 mediates adrenergic control of lipolysis by functioning as a cytosolic A-kinase anchoring protein (AKAP), on the hemimembrane that envelops the lipid droplet. This article is part of a Special Issue entitled: Mitochondrial dynamics and physiology.

Published

2013

14. Melanopsin-expressing retinal ganglion cells are resistant to cell injury, but not always

Author

Fred N. Ross-Cisneros, Alfredo A. Sadun, Valerio Carelli, Chiara La Morgia, Birgitte Georg, Jens Hannibal, Carla Giordano, Anna Ghelli, Georg, Birgitte, Ghelli, ANNA MARIA, Giordano, Carla, Ross Cisneros, Fred N., Sadun, Alfredo A., Carelli, Valerio, Hannibal, Jen, and LA MORGIA, Chiara

Subjects

0301 basic medicine, Melanopsin, Retinal Ganglion Cells, Dominant optic atrophy, Mitochondrial Diseases, Light, genetic structures, medicine.medical_treatment, Gene Expression, Mitochondrion, Biology, Retinal ganglion, Optic neuropathy, 03 medical and health sciences, 0302 clinical medicine, Leber's hereditary optic neuropathy, Stress, Physiological, Optic Nerve Diseases, Robustne, medicine, Humans, Optic atrophy, Retinal ganglion cell, Molecular Biology, Intrinsically photosensitive retinal ganglion cells, Rod Opsins, Cell Biology, Anatomy, medicine.disease, eye diseases, Mitochondria, 030104 developmental biology, Alzheimer, Molecular Medicine, sense organs, alzheimer, dominant optic atrophy, light, melanopsin, mitochondria, optic atrophy, retinal ganglion cells, robustness, molecular medicine, molecular biology, cell biology, Axotomy, Mitochondrial optic neuropathies, Neuroscience, 030217 neurology & neurosurgery

Abstract

Melanopsin retinal ganglion cells (mRGCs) are intrinsically photosensitive RGCs deputed to non-image forming functions of the eye such as synchronization of circadian rhythms to light-dark cycle. These cells are characterized by unique electrophysiological, anatomical and biochemical properties and are usually more resistant than conventional RGCs to different insults, such as axotomy and different paradigms of stress. We also demonstrated that these cells are relatively spared compared to conventional RGCs in mitochondrial optic neuropathies (Leber's hereditary optic neuropathy and Dominant Optic Atrophy). However, these cells are affected in other neurodegenerative conditions, such as glaucoma and Alzheimer's disease. We here review the current evidences that may underlie this dichotomy. We also present our unpublished data on cell experiments demonstrating that melanopsin itself does not explain the robustness of these cells and some preliminary data on immunohistochemical assessment of mitochondria in mRGCs.

Published

2016

15. The human OPA1delTTAG mutation induces premature age-related systemic neurodegeneration in mouse

Author

Jing Wang, Valérie Rigau, Guy Bielicki, Chantal Cazevieille, Marie Seveno, Jean-Luc Puel, Pascal Reynier, Naïg Gueguen, Christian P. Hamel, Anne-Laure Mausset-Bonnefont, Jean-Pierre Renou, Philippe Brabet, Benjamin Chaix, Cécile Delettre, Guy Lenaers, Nathalie Boddaert, Claire Angebault, Emmanuelle Sarzi, Université Montpellier 1 (UM1), Centre Hospitalier Universitaire d'Angers (CHU Angers), PRES Université Nantes Angers Le Mans (UNAM), Qualité des Produits Animaux (QuaPA), Institut National de la Recherche Agronomique (INRA), CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Centre Hospitalier Universitaire Gui de Chauliac (CHU Gui de Chauliac), Association Francaise contre les Myopathies, Retina France, Union Nationale des Aveugles et Deficients Visuels, Ouvrir Les Yeux, and European E-RARE program ERMION

Subjects

Retinal Ganglion Cells, CARDIOLIPIN, Pathology, Magnetic Resonance Spectroscopy, Mitochondrial Diseases, Mitochondrion, Nervous System, GTP Phosphohydrolases, Mice, FUSION, 0302 clinical medicine, [SDV.IDA]Life Sciences [q-bio]/Food engineering, Mitophagy, Sequence Deletion, 0303 health sciences, Neurodegeneration, Age Factors, neurodegeneration, Aging, Premature, DEFECTS, Magnetic Resonance Imaging, respiratory chain complexes, ALZHEIMERS-DISEASE, DEFICIENCY, mitochondria, Phenotype, OPA1 MUTATIONS, mitochondrial fusion, Disease Progression, medicine.symptom, Glycolysis, Locomotion, Psychoacoustics, medicine.medical_specialty, Ataxia, DOMINANT OPTIC ATROPHY, mouse model, Mice, Transgenic, Biology, Retinal ganglion, Retina, Electron Transport Complex IV, 03 medical and health sciences, Atrophy, Physical Conditioning, Animal, Optic Atrophy, Autosomal Dominant, Electroretinography, Evoked Potentials, Auditory, Brain Stem, Reaction Time, medicine, Animals, Humans, [SPI.GPROC]Engineering Sciences [physics]/Chemical and Process Engineering, Lactic Acid, Muscle, Skeletal, 030304 developmental biology, Aspartic Acid, Chi-Square Distribution, Membrane Proteins, Optic Nerve, MITOCHONDRIAL-DNA INSTABILITY, IN-VITRO, Creatine, medicine.disease, eye diseases, Mice, Inbred C57BL, MODEL, Disease Models, Animal, Peripheral neuropathy, Acoustic Stimulation, Electron Transport Chain Complex Proteins, Gene Expression Regulation, Evoked Potentials, Visual, Neurology (clinical), Psychomotor Performance, 030217 neurology & neurosurgery

Abstract

International audience; Dominant optic atrophy is a rare inherited optic nerve degeneration caused by mutations in the mitochondrial fusion gene OPA1. Recently, the clinical spectrum of dominant optic atrophy has been extended to frequent syndromic forms, exhibiting various degrees of neurological and muscle impairments frequently found in mitochondrial diseases. Although characterized by a specific loss of retinal ganglion cells, the pathophysiology of dominant optic atrophy is still poorly understood. We generated an Opa1 mouse model carrying the recurrent Opa1(delTTAG) mutation, which is found in 30% of all patients with dominant optic atrophy. We show that this mouse displays a multi-systemic poly-degenerative phenotype, with a presentation associating signs of visual failure, deafness, encephalomyopathy, peripheral neuropathy, ataxia and cardiomyopathy. Moreover, we found premature age-related axonal and myelin degenerations, increased autophagy and mitophagy and mitochondrial supercomplex instability preceding degeneration and cell death. Thus, these results support the concept that Opa1 protects against neuronal degeneration and opens new perspectives for the exploration and the treatment of mitochondrial diseases.

Published

2012

16. Mitofilin complexes: conserved organizers of mitochondrial membrane architecture

Author

Martin van der Laan, Ralf M. Zerbes, Ida J. van der Klei, Nikolaus Pfanner, Marten Veenhuis, and Maria Bohnert

Subjects

DOMINANT OPTIC ATROPHY, Translocase of the outer membrane, Clinical Biochemistry, Muscle Proteins, Biology, Models, Biological, Biochemistry, Mitochondrial Proteins, mitochondrial morphology, Mitochondrial membrane transport protein, CRISTAE MORPHOLOGY, ELECTRON TOMOGRAPHY, cristae, INNER-MEMBRANE, PROTEIN IMPORT, Animals, Humans, PROTEOMIC IDENTIFICATION, Inner membrane, DYNAMIN-RELATED GTPASE, OXIDATIVE STRESS, Inner mitochondrial membrane, Molecular Biology, Conserved Sequence, Fcj1, MINOS, TRANSLOCATION CONTACT SITES, MICOS complex, crista junction, Mitochondrial carrier, Cell biology, Mio10, Mitochondrial Membranes, RAT-BRAIN MITOCHONDRIA, Translocase of the inner membrane, biology.protein, Bacterial outer membrane

Abstract

Mitofilin proteins are crucial organizers of mitochondrial architecture. They are located in the inner mitochondrial membrane and interact with several protein complexes of the outer membrane, thereby generating contact sites between the two membrane systems of mitochondria. Within the inner membrane, mitofilins are part of hetero-oligomeric protein complexes that have been termed the mitochondrial inner membrane organizing system (MINOS). MINOS integrity is required for the maintenance of the characteristic morphology of the inner mitochondrial membrane, with an inner boundary region closely apposed to the outer membrane and cristae membranes, which form large tubular invaginations that protrude into the mitochondrial matrix and harbor the enzyme complexes of the oxidative phosphorylation machinery. MINOS deficiency comes along with a loss of crista junction structures and the detachment of cristae from the inner boundary membrane. MINOS has been conserved in evolution from unicellular eukaryotes to humans, where alterations of MINOS subunits are associated with multiple pathological conditions.

Published

2012

17. Disorders of the Optic Nerve in Mitochondrial Cytopathies: New Ideas on Pathogenesis and Therapeutic Targets

Author

Patrick Yu-Wai-Man, Kamil S. Sitarz, and Patrick F. Chinnery

Subjects

Mitochondrial DNA, medicine.medical_specialty, Mitochondrial Diseases, Dominant optic atrophy, Neurology, genetic structures, Optic nerve, Neuroscience(all), Hereditary spastic paraplegia, Heteroplasmy, Mitochondrial disease, Clinical Neurology, Neuro-Ophthalmology (G Plant, Section Editor), Biology, Neuroprotection, Haplogroup, Multiple sclerosis, Optic neuropathy, 03 medical and health sciences, 0302 clinical medicine, Optic Nerve Diseases, Medicine & Public Health, medicine, Humans, Idebenone, Retinal ganglion cell, Mitofusin, General Neuroscience, Mitochondrial cytopathies, medicine.disease, eye diseases, Mitochondria, 3. Good health, 030221 ophthalmology & optometry, Calcium, sense organs, Neurology (clinical), Mitochondrial optic neuropathies, Reactive Oxygen Species, Leber hereditary optic neuropathy, Neuroscience, 030217 neurology & neurosurgery, medicine.drug

Abstract

Mitochondrial cytopathies are a heterogeneous group of human disorders triggered by disturbed mitochondrial function. This can be due to primary mitochondrial DNA mutations or nuclear defects affecting key components of the mitochondrial machinery. Optic neuropathy is a frequent disease manifestation and the degree of visual failure can be profound, with a severe impact on the patient's quality of life. This review focuses on the major mitochondrial disorders exhibiting optic nerve involvement, either as the defining clinical feature or as an additional component of a more extensive phenotype. Over the past decade, significant progress has been achieved in our basic understanding of Leber hereditary optic neuropathy and autosomal-dominant optic atrophy--the two classical paradigms for these mitochondrial optic neuropathies. There are currently limited treatments for these blinding ocular disorders and, ultimately, the aim is to translate these major advances into tangible benefits for patients and their families.

Published

2012

18. Mitochondrial optic neuropathies – Disease mechanisms and therapeutic strategies

Author

Patrick Yu-Wai-Man, Patrick F. Chinnery, and Philip G. Griffiths

Subjects

Mitochondrial DNA, Dominant optic atrophy, genetic structures, Hereditary spastic paraplegia, Respiratory chain, Optic neuritis, Optic neuropathy, Biology, Retinal ganglion, Article, Multiple sclerosis, 03 medical and health sciences, 0302 clinical medicine, medicine, Retinal ganglion cell, Mitofusin, Inner mitochondrial membrane, Leber's hereditary optic neuropathy, Glaucoma, medicine.disease, Neuroprotection, eye diseases, Sensory Systems, 3. Good health, Ophthalmology, 030221 ophthalmology & optometry, Optic nerve, sense organs, Mitochondrial optic neuropathies, Leber hereditary optic neuropathy, Neuroscience, 030217 neurology & neurosurgery

Abstract

Leber hereditary optic neuropathy (LHON) and autosomal-dominant optic atrophy (DOA) are the two most common inherited optic neuropathies in the general population. Both disorders share striking pathological similarities, marked by the selective loss of retinal ganglion cells (RGCs) and the early involvement of the papillomacular bundle. Three mitochondrial DNA (mtDNA) point mutations; m.3460G>A, m.11778G>A, and m.14484T>C account for over 90% of LHON cases, and in DOA, the majority of affected families harbour mutations in the OPA1 gene, which codes for a mitochondrial inner membrane protein. Optic nerve degeneration in LHON and DOA is therefore due to disturbed mitochondrial function and a predominantly complex I respiratory chain defect has been identified using both in vitro and in vivo biochemical assays. However, the trigger for RGC loss is much more complex than a simple bioenergetic crisis and other important disease mechanisms have emerged relating to mitochondrial network dynamics, mtDNA maintenance, axonal transport, and the involvement of the cytoskeleton in maintaining a differential mitochondrial gradient at sites such as the lamina cribosa. The downstream consequences of these mitochondrial disturbances are likely to be influenced by the local cellular milieu. The vulnerability of RGCs in LHON and DOA could derive not only from tissue-specific, genetically-determined biological factors, but also from an increased susceptibility to exogenous influences such as light exposure, smoking, and pharmacological agents with putative mitochondrial toxic effects. Our concept of inherited mitochondrial optic neuropathies has evolved over the past decade, with the observation that patients with LHON and DOA can manifest a much broader phenotypic spectrum than pure optic nerve involvement. Interestingly, these phenotypes are sometimes clinically indistinguishable from other neurodegenerative disorders such as Charcot-Marie-Tooth disease, hereditary spastic paraplegia, and multiple sclerosis, where mitochondrial dysfunction is also thought to be an important pathophysiological player. A number of vertebrate and invertebrate disease models has recently been established to circumvent the lack of human tissues, and these have already provided considerable insight by allowing direct RGC experimentation. The ultimate goal is to translate these research advances into clinical practice and new treatment strategies are currently being investigated to improve the visual prognosis for patients with mitochondrial optic neuropathies.

Published

2011

19. Neuroradiological findings expand the phenotype of OPA1-related mitochondrial dysfunction

Author

Michel Pagès, Catherine Blanchet, Christian P. Hamel, H. Brunel, Agathe Roubertie, Gaël Manes, Emmanuelle Le Bars, Michel Mondain, Marie Christine Picot, Guy Lenaers, Claire Angebault Prouteau, Nicolas Leboucq, Erika Nogue, Hugues Chevassus, Emmanuelle Sarzi, Isabelle Meunier, Max Villain, Patrizia Amati-Bonneau, Biologie Neurovasculaire et Mitochondriale Intégrée (BNMI), Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Institut des Neurosciences de Montpellier - Déficits sensoriels et moteurs (INM), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Montpellier (UM), CHU de Montpellier, and Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier)

Subjects

Male, Pathology, medicine.medical_specialty, Magnetic Resonance Spectroscopy, Visual acuity, Mitochondrial Diseases, Adolescent, Optic nerve, [SDV]Life Sciences [q-bio], Brain imaging, Neurological examination, Fluid-attenuated inversion recovery, Motor Activity, OPA1, Retinal ganglion, GTP Phosphohydrolases, White matter, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Atrophy, Optic Atrophy, Autosomal Dominant, medicine, Humans, dominant optic atrophy, Child, Hearing Loss, 030304 developmental biology, Neurologic Examination, Mitochondrial disorders, 0303 health sciences, medicine.diagnostic_test, business.industry, Brain, medicine.disease, Magnetic Resonance Imaging, eye diseases, 3. Good health, medicine.anatomical_structure, Neurology, Child, Preschool, Cerebellar atrophy, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

International audience; OBJECTIVE: OPA1 mutations are responsible for more than half of autosomal dominant optic atrophy (ADOA), a blinding disease affecting the retinal ganglion neurons. In most patients the clinical presentation is restricted to the optic nerve degeneration, albeit in 20% of them, additional neuro-sensorial symptoms might be associated to the loss of vision, as frequently encountered in mitochondrial diseases. This study describes clinical and neuroradiological features of OPA1 patients.METHODS: Twenty two patients from 17 families with decreased visual acuity related to optic atrophy and carrying an OPA1 mutation were enrolled. Patients underwent neuro-ophthalmological examinations. Brain magnetic resonance imaging (T1, T2 and flair sequences) was performed on a 1.5-Tesla MR Unit. Twenty patients underwent 2-D proton spectroscopic imaging.RESULTS: Brain imaging disclosed abnormalities in 12 patients. Cerebellar atrophy mainly involving the vermis was observed in almost a quarter of the patients; other abnormalities included unspecific white matter hypersignal, hemispheric cortical atrophy, and lactate peak. Neurological examination disclosed one patient with a transient right hand motor deficit and ENT examination revealed hearing impairment in 6 patients. Patients with abnormal MRI were characterized by: (i) an older age (ii) more severe visual impairment with chronic visual acuity deterioration, and (iii) more frequent associated deafness.CONCLUSIONS: Our results demonstrate that brain imaging abnormalities are common in OPA1 patients, even in those with normal neurological examination. Lactate peak, cerebellar and cortical atrophies are consistent with the mitochondrial dysfunction related to OPA1 mutations and might result from widespread neuronal degeneration.

Published

2014

20. Colour discrimination ellipses in patients with dominant optic atrophy

Author

B. C. Regan, Matthew P. Simunovic, Marcela Votruba, and John D. Mollon

Subjects

Adult, Male, medicine.medical_specialty, Dominant optic atrophy, Visual acuity, genetic structures, Color vision, Visual Acuity, Color Vision Defects, Colour vision deficiency, Audiology, Colour discrimination, Vision disorder, Atrophy, Optics, Optic Atrophies, Hereditary, medicine, Humans, In patient, Chromatic scale, Low vision, Aged, Color Perception Tests, business.industry, Middle Aged, medicine.disease, eye diseases, Sensory Systems, Ophthalmology, Sensory Thresholds, Optic nerve, Female, medicine.symptom, business, Psychology

Abstract

Many colour tests require a visual acuity of at least 0.1, making them unsuitable for low vision patients. To assess colour vision in patients with sub-normal acuity, we re-designed a previously described test so that its spatial details would be coarse enough to be resolvable by subjects with severe visual impairment. The test measures chromatic discrimination along 20 axes evenly spaced in CIE 1976 L*u*v* colour space. We detail the results for this test in a group of patients with dominant optic atrophy. Despite the lack of evidence for genetic heterogeneity in dominant optic atrophy, we observed phenotypic variation both between and within families.

Published

1998

21. Listeria monocytogenes transiently alters mitochondrial dynamics during infection

Author

Fabrizia Stavru, Frédéric Bouillaud, Daniel Ricquier, Pascale Cossart, Anna Sartori, USC2020, Inst Natl Rech Agron, Interactions Bactéries-Cellules (UIBC), Institut National de la Recherche Agronomique (INRA)-Institut Pasteur [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), Université Paris Descartes - Paris 5 (UPD5), Institut Pasteur [Paris], European Research Council [233348], Fondation Le Roch Les Mousquetaires, Fondation Jeantet, Roux Fellowship (Institut Pasteur), Institut National de la Recherche Agronomique (INRA)-Institut Pasteur [Paris] (IP)-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut Cochin (IC UM3 (UMR 8104 / U1016)), Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Microscopie ultrastructurale (plate-forme), Institut Pasteur [Paris] (IP), and European Project: 233348,EC:FP7:ERC,ERC-2008-AdG,MODELIST(2009)

Subjects

DOMINANT OPTIC ATROPHY, [SDV]Life Sciences [q-bio], Bacterial Toxins, Cell Respiration, Intracellular Space, PROTEIN, Apoptosis, Mitochondrion, Listeria infection, medicine.disease_cause, bioenergetics, Microbiology, 03 medical and health sciences, Hemolysin Proteins, FUSION, Adenosine Triphosphate, Listeria monocytogenes, Heat shock protein, MAMMALIAN HOMOLOGS, medicine, Humans, Listeriosis, Heat-Shock Proteins, 030304 developmental biology, Membrane Potential, Mitochondrial, 0303 health sciences, Multidisciplinary, DIVISION, biology, Intracellular parasite, 030302 biochemistry & molecular biology, Listeriolysin O, bacterial infection, Biological Sciences, medicine.disease, biology.organism_classification, FISSION, Cell biology, Mitochondria, mitochondrial fusion, CELLS, Listeria, Potassium, Calcium, calcium influx, HISTONE MODIFICATIONS, HeLa Cells

Abstract

Mitochondria are essential and highly dynamic organelles, constantly undergoing fusion and fission. We analyzed mitochondrial dynamics during infection with the human bacterial pathogen Listeria monocytogenes and show that this infection profoundly alters mitochondrial dynamics by causing transient mitochondrial network fragmentation. Mitochondrial fragmentation is specific to pathogenic Listeria monocytogenes , and it is not observed with the nonpathogenic Listeria innocua species or several other intracellular pathogens. Strikingly, the efficiency of Listeria infection is affected in cells where either mitochondrial fusion or fission has been altered by siRNA treatment, highlighting the relevance of mitochondrial dynamics for Listeria infection. We identified the secreted pore-forming toxin listeriolysin O as the bacterial factor mainly responsible for mitochondrial network disruption and mitochondrial function modulation. Together, our results suggest that the transient shutdown of mitochondrial function and dynamics represents a strategy used by Listeria at the onset of infection to interfere with cellular physiology.

Published

2011

22. Retinal nerve fiber layer thickness in dominant optic atrophy measurements by optical coherence tomography and correlation with age

Author

Barboni P., Savini G., Parisi V., Carbonelli M., Sadun F., De Negri A. M., Carta A., Sadun A. A., LA MORGIA, CHIARA, MARESCA, ALESSANDRA, CARELLI, VALERIO, Barboni P., Savini G., Parisi V., Carbonelli M., La Morgia C., Maresca A., Sadun F., De Negri A.M., Carta A., Sadun A.A., and Carelli V.

Subjects

Adult, Retinal Ganglion Cells, Aging, genetic structures, Adolescent, Optic Disk, Visual Acuity, DOA, OPA1, GTP Phosphohydrolases, Nerve Fibers, Optic Atrophy, Autosomal Dominant, Humans, dominant optic atrophy, Child, Aged, optical coherence tomography, Middle Aged, eye diseases, Pedigree, mitochondria, Retinal nerve fiber layer, Cross-Sectional Studies, RNFL, Mutation, sense organs, Tomography, Optical Coherence

Abstract

To measure the retinal nerve fiber layer (RNFL) thickness by means of optical coherence tomography (OCT) in patients with dominant optic atrophy (DOA).Cross-sectional study.Thirty-three patients from 15 pedigrees with DOA harboring heterozygous mutations in the OPA1 gene and 43 healthy subjects were enrolled.The RNFLs of DOA patients were studied by OCT and compared with those of 43 healthy subjects matched for age and optic nerve head (ONH) size.Retinal nerve fiber layer thickness.Dominant optic atrophy patients revealed a significant RNFL thickness reduction in all quadrants, with a preferential involvement of the temporal and inferior sectors. The progressive decline of RNFL thickness with age was similar to that observed in healthy subjects and was more evident in the 2 quadrants with higher residual amounts of fibers, that is, the superior and the inferior. The temporal quadrant was profoundly depleted of fiber so that the further rate of loss of microns per year is close to zero, whereas the nasal quadrant was spared the most by neurodegeneration.The present findings, taken in conjunction with the authors' previous description of small ONH size in DOA, strongly suggest that patients with this disease are born with fewer optic nerve axons and support the hypothesis that subsequent visual loss depends on further age-related loss of fibers, which also occurs in controls.The author(s) have no proprietary or commercial interest in any materials discussed in this article.

Published

2010

23. A novel deletion in the GTPase domain of OPA1 causes defects in mitochondrial morphology and distribution, but not in function

Author

Christian Frezza, Luca Scorrano, Alessandra Baracca, Corrado Angelini, Leonardo Salviati, Giancarlo Solaini, Giovanna Cenacchi, Gabriella Casalena, Adriana Malena, Mario Bortolozzi, Gianluca Sgarbi, Alberto Casarin, Silvia Cazzola, Emanuele Loro, Marco Spinazzi, Franco Carrara, Lodovica Vergani, Spinazzi M, Cazzola S, Bortolozzi M, Baracca A, Loro E, Casarin A, Solaini G, Sgarbi G, Casalena G, Cenacchi G, Malena A, Frezza C, Carrara F, Angelini C, Scorrano L, Salviati L, and Vergani L.

Subjects

Male, Apoptosis, Mitochondrion, medicine.disease_cause, OPA1, GTP Phosphohydrolases, Pathogenesis, FUSION, CULTURED MUSCLE, Child, MUTATION, DYNAMIN RELATED PROTEIN, Genetics (clinical), Cells, Cultured, Sequence Deletion, Genetics, Mutation, MITOCHONDRIAL DYNAMICS, Myogenesis, Retina/pathology, General Medicine, Optic Atrophy, Autosomal Dominant/*genetics/physiopathology, Middle Aged, Muscle, Skeletal/abnormalities/enzymology, Cell biology, COMPLEX I DEFICIENCY, Mitochondria, Pedigree, medicine.anatomical_structure, Retinal ganglion cell, RESPIRATION, Optic Atrophy 1, Female, Mitochondria/*metabolism/pathology, Adult, Adolescent, DOMINANT OPTIC ATROPHY, Biology, Gene Expression Regulation, Enzymologic, Retina, Young Adult, Atrophy, Reactive Oxygen Species/metabolism, Optic Atrophy, Autosomal Dominant, medicine, Humans, ddc:612, Muscle, Skeletal, Molecular Biology, PROTEOLYTIC CLEAVAGE, GTP Phosphohydrolases/*genetics/metabolism, MTDNA MAINTENANCE, MUTATIONS, medicine.disease, APOPTOSIS, DYSFUNCTION, eye diseases, MORPHOLOGY, sense organs, Energy Metabolism, Reactive Oxygen Species

Abstract

Autosomal dominant optic atrophy (ADOA), the commonest cause of inherited optic atrophy, is caused by mutations in the ubiquitously expressed gene optic atrophy 1 (OPA1), involved in fusion and biogenesis of the inner membrane of mitochondria. Bioenergetic failure, mitochondrial network abnormalities and increased apoptosis have all been proposed as possible causal factors. However, their relative contribution to pathogenesis as well as the prominent susceptibility of the retinal ganglion cell (RGC) in this disease remains uncertain. Here we identify a novel deletion of OPA1 gene in the GTPase domain in three patients affected by ADOA. Muscle biopsy of the patients showed neurogenic atrophy and abnormal morphology and distribution of mitochondria. Confocal microscopy revealed increased mitochondrial fragmentation in fibroblasts as well as in myotubes, where mitochondria were also unevenly distributed, with clustered organelles alternating with areas where mitochondria were sparse. These abnormalities were not associated with altered bioenergetics or increased susceptibility to pro-apoptotic stimuli. Therefore, changes in mitochondrial shape and distribution can be independent of other reported effects of OPA1 mutations, and therefore may be the primary cause of the disease. The arrangement of mitochondria in RGCs, which degenerate in ADOA, may be exquisitely sensitive to disturbance, and this may lead to bioenergetic crisis and/or induction of apoptosis. Our results highlight the importance of mitochondrial dynamics in the disease per se, and point to the loss of the fine positioning of mitochondria in the axons of RGCs as a possible explanation for their predominant degeneration in ADOA.

Published

2008