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MSTO1 mutations cause mtDNA depletion, manifesting as muscular dystrophy with cerebellar involvement.
Donkervoort, S; Sabouny, R; Yun, P; Gauquelin, L; Chao, K R; Hu, Y; Al Khatib, I; Töpf, A; Mohassel, P; Cummings, B B; Kaur, R; Saade, D; Moore, S A; Waddell, L B; Farrar, M A; Goodrich, J K; Uapinyoying, P; Chan, S H S; Javed, A; Leach, M E; Karachunski, P; Dalton, J; Medne, L; Harper, A; Thompson, C; Thiffault, I; Specht, S; Lamont, R E; Saunders, C; Racher, H; Bernier, F P; Mowat, D; Witting, N; Vissing, J; Hanson, R; Coffman, K A; Hainlen, M; Parboosingh, J S; Carnevale, A; Yoon, G; Schnur, R E; Boycott, K M; Mah, J K; Straub, V; Foley, A Reghan; Innes, A M; Bönnemann, C G; Shutt, T E.
Affiliation
  • Donkervoort S; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Sabouny R; Department of Biochemistry and Molecular Biology, University of Calgary, Calgary, Canada.
  • Yun P; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Gauquelin L; Division of Clinical and Metabolic Genetics, Department of Paediatrics, The Hospital for Sick Children, University of Toronto, Toronto, ON, Canada.
  • Chao KR; Division of Neurology, Department of Paediatrics, The Hospital for Sick Children, University of Toronto, Toronto, ON, Canada.
  • Hu Y; Center for Mendelian Genomics, Program in Medical and Population Genetics, Broad Institute of MIT and Harvard, Boston, MA, USA.
  • Al Khatib I; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Töpf A; Department of Biochemistry and Molecular Biology, University of Calgary, Calgary, Canada.
  • Mohassel P; John Walton Muscular Dystrophy Research Centre, Institute of Genetic Medicine, Newcastle University, Newcastle upon Tyne, UK.
  • Cummings BB; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Kaur R; Center for Mendelian Genomics, Program in Medical and Population Genetics, Broad Institute of MIT and Harvard, Boston, MA, USA.
  • Saade D; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Moore SA; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Waddell LB; Department of Pathology Carver College of Medicine, The University of Iowa, Iowa City, IA, USA.
  • Farrar MA; Kids Neuroscience Centre, Kids Research, The Children's Hospital at Westmead, Sydney, NSW 2145, Australia.
  • Goodrich JK; Discipline of Child and Adolescent Health, Faculty of Medicine and Health, The University of Sydney, Westmead, NSW 2145, Australia.
  • Uapinyoying P; Department of Neurology, Sydney Children's Hospital, Sydney, NSW, Australia.
  • Chan SHS; UNSW Sydney, School of Women's and Children's Health, Sydney, NSW, Australia.
  • Javed A; Center for Mendelian Genomics, Program in Medical and Population Genetics, Broad Institute of MIT and Harvard, Boston, MA, USA.
  • Leach ME; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Karachunski P; Research for Genetic Medicine, Children's National Medical Center, Washington, DC, USA.
  • Dalton J; Department of Paediatrics and Adolescent Medicine, Queen Mary Hospital, The University of Hong Kong, Hong Kong SAR, China.
  • Medne L; School of Biomedical Science, The University of Hong Kong, Hong Kong SAR, China.
  • Harper A; Neuromuscular and Neurogenetic Disorders of Childhood Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD, USA.
  • Thompson C; Oregon Health and Science University, Neuromuscular Program, Doernbecher Children's Hospital, Portland, OR, USA.
  • Thiffault I; Department of Neurology, University of Minnesota, Minneapolis, MN, USA.
  • Specht S; Department of Neurology, University of Minnesota, Minneapolis, MN, USA.
  • Lamont RE; Division of Human Genetics, The Children's Hospital of Philadelphia, Philadelphia, USA.
  • Saunders C; Department of Neurology, Virginia Commonwealth University, Children's Hospital of Richmond at VCU, Richmond, VA, USA.
  • Racher H; Department of Pediatrics, University of California San Diego, San Diego, CA, USA.
  • Bernier FP; Department of Pathology and Laboratory Medicine, Children's Mercy Hospital, Kansas City, USA.
  • Mowat D; Center for Pediatric Genomic Medicine, Children's Mercy Hospital, Kansas City, USA.
  • Witting N; University of Missouri-Kansas City School of Medicine, Kansas City, USA.
  • Vissing J; John Walton Muscular Dystrophy Research Centre, Institute of Genetic Medicine, Newcastle University, Newcastle upon Tyne, UK.
  • Hanson R; Department of Medical Genetics and Alberta Children's Hospital Research Institute, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.
  • Coffman KA; Department of Pathology and Laboratory Medicine, Children's Mercy Hospital, Kansas City, USA.
  • Hainlen M; Center for Pediatric Genomic Medicine, Children's Mercy Hospital, Kansas City, USA.
  • Parboosingh JS; University of Missouri-Kansas City School of Medicine, Kansas City, USA.
  • Carnevale A; Department of Medical Genetics and Alberta Children's Hospital Research Institute, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.
  • Yoon G; Department of Medical Genetics and Alberta Children's Hospital Research Institute, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.
  • Schnur RE; UNSW Sydney, School of Women's and Children's Health, Sydney, NSW, Australia.
  • Boycott KM; Department of Neurology, University Hospital Rigshospitalet, Copenhagen, Denmark.
  • Mah JK; Department of Neurology, University Hospital Rigshospitalet, Copenhagen, Denmark.
  • Straub V; University of Missouri-Kansas City School of Medicine, Kansas City, USA.
  • Foley AR; Department of Pediatrics, Children's Mercy Hospital, Kansas City, USA.
  • Innes AM; Department of Pediatrics, Children's Mercy Hospital, Kansas City, USA.
  • Bönnemann CG; Division of Neurology, Children's Mercy Hospital, Kansas City, USA.
  • Shutt TE; Department of Pediatrics, Children's Mercy Hospital, Kansas City, USA.
Acta Neuropathol ; 138(6): 1013-1031, 2019 12.
Article de En | MEDLINE | ID: mdl-31463572
ABSTRACT
MSTO1 encodes a cytosolic mitochondrial fusion protein, misato homolog 1 or MSTO1. While the full genotype-phenotype spectrum remains to be explored, pathogenic variants in MSTO1 have recently been reported in a small number of patients presenting with a phenotype of cerebellar ataxia, congenital muscle involvement with histologic findings ranging from myopathic to dystrophic and pigmentary retinopathy. The proposed underlying pathogenic mechanism of MSTO1-related disease is suggestive of impaired mitochondrial fusion secondary to a loss of function of MSTO1. Disorders of mitochondrial fusion and fission have been shown to also lead to mitochondrial DNA (mtDNA) depletion, linking them to the mtDNA depletion syndromes, a clinically and genetically diverse class of mitochondrial diseases characterized by a reduction of cellular mtDNA content. However, the consequences of pathogenic variants in MSTO1 on mtDNA maintenance remain poorly understood. We present extensive phenotypic and genetic data from 12 independent families, including 15 new patients harbouring a broad array of bi-allelic MSTO1 pathogenic variants, and we provide functional characterization from seven MSTO1-related disease patient fibroblasts. Bi-allelic loss-of-function variants in MSTO1 manifest clinically with a remarkably consistent phenotype of childhood-onset muscular dystrophy, corticospinal tract dysfunction and early-onset non-progressive cerebellar atrophy. MSTO1 protein was not detectable in the cultured fibroblasts of all seven patients evaluated, suggesting that pathogenic variants result in a loss of protein expression and/or affect protein stability. Consistent with impaired mitochondrial fusion, mitochondrial networks in fibroblasts were found to be fragmented. Furthermore, all fibroblasts were found to have depletion of mtDNA ranging from 30 to 70% along with alterations to mtDNA nucleoids. Our data corroborate the role of MSTO1 as a mitochondrial fusion protein and highlight a previously unrecognized link to mtDNA regulation. As impaired mitochondrial fusion is a recognized cause of mtDNA depletion syndromes, this novel link to mtDNA depletion in patient fibroblasts suggests that MSTO1-deficiency should also be considered a mtDNA depletion syndrome. Thus, we provide mechanistic insight into the disease pathogenesis associated with MSTO1 mutations and further define the clinical spectrum and the natural history of MSTO1-related disease.
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Texte intégral: 1 Collection: 01-internacional Base de données: MEDLINE Sujet principal: ADN mitochondrial / Maladies du cervelet / Protéines du cycle cellulaire / Maladies mitochondriales / Protéines du cytosquelette / Dystrophies musculaires / Mutation Limites: Adolescent / Adult / Child / Female / Humans / Male / Middle aged Langue: En Journal: Acta Neuropathol Année: 2019 Type de document: Article Pays d'affiliation: États-Unis d'Amérique
Texte intégral
Ajouter à My VHL
Imprimer
XML
PubMed Links
Recherche sur Google

Texte intégral: 1 Collection: 01-internacional Base de données: MEDLINE Sujet principal: ADN mitochondrial / Maladies du cervelet / Protéines du cycle cellulaire / Maladies mitochondriales / Protéines du cytosquelette / Dystrophies musculaires / Mutation Limites: Adolescent / Adult / Child / Female / Humans / Male / Middle aged Langue: En Journal: Acta Neuropathol Année: 2019 Type de document: Article Pays d'affiliation: États-Unis d'Amérique