For Publishers
DiscoveryMetadataPeer reviewHostingPublishing
For Researchers
JoinPublishReviewCollect
Register
Blog
About
Search
Advanced search
My ScienceOpen
Search
For Publishers
For Researchers
Blog
About
78
views
57
references
 Top references
cited by
73
    
0 reviews
 Review
0
comments
 Comment
0
recommends
+1 Recommend
0 collections
    0
    shares
      314
      similar
       All similar
      • Record: found
      • Abstract: found
      • Article: found
      Is Open Access

      Multi-system neurological disease is common in patients with OPA1 mutations

      research-article
      Author(s): 1 , 2 , 1 , 2 , 1 , 3 , 4 , 5 , 6 , 6 , 7 , 7 , 8 , 9 , 10 , 11 , 1 , 11 , 12 , 11 , 2 , 13 , 14 , 1 , 1 , 15 , 16 , 15 , 16 , 3 , 17 , 1 , 1 , 1 , 18 , 19 , 8 , 7 , 20 , 21 ,   1 , 22 , 15 , 16 , 1 , 23 ,
      Publication date (Electronic):
      Journal: Brain
      Publisher: Oxford University Press
      Keywords: deletions, dominant optic atrophy, hereditary spastic paraplegia, mitochondrial DNA, multiple sclerosis, OPA1

      Read this article at

      ScienceOpenPublisherPMC
      Bookmark
          There is no author summary for this article yet. Authors can add summaries to their articles on ScienceOpen to make them more accessible to a non-specialist audience.

          Abstract

          Additional neurological features have recently been described in seven families transmitting pathogenic mutations in OPA1, the most common cause of autosomal dominant optic atrophy. However, the frequency of these syndromal ‘dominant optic atrophy plus’ variants and the extent of neurological involvement have not been established. In this large multi-centre study of 104 patients from 45 independent families, including 60 new cases, we show that extra-ocular neurological complications are common in OPA1 disease, and affect up to 20% of all mutational carriers. Bilateral sensorineural deafness beginning in late childhood and early adulthood was a prominent manifestation, followed by a combination of ataxia, myopathy, peripheral neuropathy and progressive external ophthalmoplegia from the third decade of life onwards. We also identified novel clinical presentations with spastic paraparesis mimicking hereditary spastic paraplegia, and a multiple sclerosis-like illness. In contrast to initial reports, multi-system neurological disease was associated with all mutational subtypes, although there was an increased risk with missense mutations [odds ratio = 3.06, 95% confidence interval = 1.44–6.49; P = 0.0027], and mutations located within the guanosine triphosphate-ase region (odds ratio = 2.29, 95% confidence interval = 1.08–4.82; P = 0.0271). Histochemical and molecular characterization of skeletal muscle biopsies revealed the presence of cytochrome c oxidase-deficient fibres and multiple mitochondrial DNA deletions in the majority of patients harbouring OPA1 mutations, even in those with isolated optic nerve involvement. However, the cytochrome c oxidase-deficient load was over four times higher in the dominant optic atrophy + group compared to the pure optic neuropathy group, implicating a causal role for these secondary mitochondrial DNA defects in disease pathophysiology. Individuals with dominant optic atrophy plus phenotypes also had significantly worse visual outcomes, and careful surveillance is therefore mandatory to optimize the detection and management of neurological disability in a group of patients who already have significant visual impairment.

          Related collections

          Most cited references57

          • Record: found
          • Abstract: not found
          • Article: not found

          Migraine--current understanding and treatment.

          Peter J Goadsby, Richard Lipton, Michel D. Ferrari (2002)
          Article 0 comments Cited 270 times – based on 0 reviews     Review now
            Bookmark
            • Record: found
            • Abstract: found
            • Article: not found

            Resolving the clinical acuity categories "hand motion" and "counting fingers" using the Freiburg Visual Acuity Test (FrACT).

            C. Lange, N Feltgen, B. Junker (2009)
            The Freiburg Visual Acuity Test (FrACT) has been suggested as a promising test for quantifying the visual acuity (VA) of patients with very low vision, a condition often classified using the semi-quantitative clinical scale "counting fingers" (CF), "hand motion" (HM), "light perception" (LP) and "no light perception". The present study was designed to assess FrACT performance in a sizable number of CF, HM, and LP patients in order to generate a setting for future clinical studies in the low vision range. We examined a total of 41 patients (LP, n = 11; CF, n = 15; HM, n = 15) with various eye diseases (e.g., diabetic retinopathy, ARMD), covering the clinical VA scale from LP to CF. The FrACT optotypes were presented at a distance of 50 cm on a 17-inch LCD monitor with four random orientations. After training, two FrACT measurements (test and retest) were taken, each comprising 30 trials. FrACT measures reproducibly the VA of CF and HM patients. In CF patients, FrACT resulted in a mean logMAR = 1.98 +/- 0.24 (corresponding to a decimal VA of 0.010), for HM in a mean logMAR = 2.28 +/- 0.15 (corresponding to a decimal VA of 0.0052). In all LP patients the FrACT values were close to what would be obtained by random guessing. The mean test-retest 95% confidence interval was 0.21 logMAR for CF patients and 0.31 logMAR for HM respectively. Test-retest variability declined from 24 to 30 trials, showing that at least 30 trials are necessary. FrACT can reproducibly quantify VA in the CF and HM range. We observed a floor effect for LP, and it was not quantifiable further. Quantitative VA measures are thus obtainable in the very low-vision range using FrACT.
            Article 0 comments Cited 166 times – based on 0 reviews     Review now
              Bookmark
              • Record: found
              • Abstract: found
              • Article: not found

              Hereditary spastic paraplegia: clinical features and pathogenetic mechanisms.

              Sara Salinas, Christos Proukakis, Andrew Crosby (2008)
              Hereditary spastic paraplegia (HSP) describes a heterogeneous group of genetic neurodegenerative disorders in which the most severely affected neurons are those of the spinal cord. These disorders are characterised clinically by progressive spasticity and weakness of the lower limbs, and pathologically by retrograde axonal degeneration of the corticospinal tracts and posterior columns. In recent years, genetic studies have identified key cellular functions that are vital for the maintenance of axonal homoeostasis in HSP. Here, we describe the clinical and diagnostic features of the various forms of HSP. We also discuss the genes that have been identified and the emerging pathogenic mechanisms.
              Article 0 comments Cited 147 times – based on 0 reviews     Review now
                Bookmark
                All references

                Author and article information

                Journal
                Journal ID (nlm-ta): Brain
                Journal ID (publisher-id): brainj
                Journal ID (hwp): brain
                Title: Brain
                Publisher: Oxford University Press
                ISSN (Print): 0006-8950
                ISSN (Electronic): 1460-2156
                Publication date (Print): March 2010
                Publication date (Electronic): 15 February 2010
                Publication date PMC-release: 15 February 2010
                Volume: 133
                Issue: 3
                Pages: 771-786
                Affiliations
                1 Mitochondrial Research Group, Institute for Ageing and Health, The Medical School, Newcastle University, UK
                2 Department of Ophthalmology, Royal Victoria Infirmary, Newcastle upon Tyne, UK
                3 Neuroscience Department, School of Medicine of Ribeirao Preto, University of Sao Paulo, Brazil
                4 MRC Human Genetics Unit, Institute of Genetics and Molecular Medicine, Western General Hospital, Edinburgh, UK
                5 Institute of Human Genetics and University Clinic of Internal Medicine, Division of Endocrinology and Nuclear Medicine, Medical University of Graz, Austria
                6 Department of Neuroscience, Psychiatry and Anaesthesiology, University of Messina, Messina, Italy
                7 Dipartimento di Scienze Neurologiche, Università di Bologna, Bologna, Italy
                8 Unit of Molecular Neurogenetics, Pierfranco and Luisa Mariani Center for the Study of Children’s Mitochondrial Disorders, National Neurological Institute, Milan, Italy
                9 Ullevål Department of Neurology, Oslo University Hospital, Oslo, Norway, UK
                10 Department of Neurology, York Hospital, York, UK
                11 Department of Neurology, Royal Victoria Infirmary, Newcastle upon Tyne, UK
                12 Institute of Neuroscience, The Medical School, Newcastle University, UK
                13 Princess Alexandra Eye Pavilion, Edinburgh, UK
                14 Medical Genetic Center MGZ, Munich, Germany
                15 Département de Biochimie et Génétique, Centre Hospitalier Universitaire d’Angers, Angers, France
                16 INSERM U-694, Angers, France
                17 INSERM U-583, Institut des Neurosciences de Montpellier, Université de Montpellier I et II, Montpellier, France
                18 School of Optometry and Vision Sciences, Cardiff University, Cardiff, UK
                19 Cardiff Eye Unit, University Hospital of Wales, Cardiff, UK
                20 Department of Clinical Medicine, University of Bergen, Bergen, Norway
                21 Department of Neurology, Haukeland University Hospital, Bergen, Norway
                22 Department of Neurology, Friedrich-Baur-Institute, Ludwig Maximilians University, Munich, Germany
                23 Institute of Human Genetics, Newcastle University, UK
                Author notes
                Correspondence to: Professor Patrick Francis Chinnery, Mitochondrial Research Group, The Medical School, Newcastle University, Newcastle upon Tyne, NE2 4HH, UK E-mail: p.f.chinnery@ 123456ncl.ac.uk
                Article
                Publisher ID: awq007
                DOI: 10.1093/brain/awq007
                PMC ID: 2842512
                PubMed ID: 20157015
                SO-VID: 5ab8dc83-e6e6-483a-96de-8ce9da04c216
                Copyright © © The Author(s) 2010. Published by Oxford University Press on behalf of Brain.
                License:

                This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License ( http://creativecommons.org/licenses/by-nc/2.5), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

                History
                Date received : 11 November 2009
                Date revision received : 15 December 2009
                Date accepted : 16 December 2009
                Categories
                Subject: Original Articles

                ScienceOpen disciplines: Neurosciences
                Keywords: opa1,deletions,multiple sclerosis,mitochondrial dna,dominant optic atrophy,hereditary spastic paraplegia
                Data availability:
                ScienceOpen disciplines: Neurosciences
                Keywords: opa1, deletions, multiple sclerosis, mitochondrial dna, dominant optic atrophy, hereditary spastic paraplegia

                Comments

                Comment on this article

                scite_

                Similar content314

                See all similar

                Cited by140

                See all cited by