Muscle & Nerve
Volume 55, Issue 6 pp. 919-922
Case of the Month

Severe defect in mitochondrial complex I assembly with mitochondrial DNA deletions in ACAD9-deficient mild myopathy

Konstantina Fragaki PhD

Konstantina Fragaki PhD

Nice Sophia Antipolis University, Institute for Research on Cancer and Aging (IRCAN), CNRS, INSERM, UMR 7284 and U1081, School of Medicine, 28 avenue de Valombrose, 06107 Nice cedex 2, France

Department of Medical Genetics, National Centre for Mitochondrial Diseases, Nice Teaching Hospital, Nice, France

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Annabelle Chaussenot MD

Annabelle Chaussenot MD

Nice Sophia Antipolis University, Institute for Research on Cancer and Aging (IRCAN), CNRS, INSERM, UMR 7284 and U1081, School of Medicine, 28 avenue de Valombrose, 06107 Nice cedex 2, France

Department of Medical Genetics, National Centre for Mitochondrial Diseases, Nice Teaching Hospital, Nice, France

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Audrey Boutron MD

Audrey Boutron MD

Department of Biochemistry, Bicetre Hospital, Assistance Publique des Hôpitaux de Paris (AP-HP), Paris-Sud Teaching Hospital, Paris, France

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Sylvie Bannwarth PhD

Sylvie Bannwarth PhD

Nice Sophia Antipolis University, Institute for Research on Cancer and Aging (IRCAN), CNRS, INSERM, UMR 7284 and U1081, School of Medicine, 28 avenue de Valombrose, 06107 Nice cedex 2, France

Department of Medical Genetics, National Centre for Mitochondrial Diseases, Nice Teaching Hospital, Nice, France

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Charlotte Cochaud CT

Charlotte Cochaud CT

Department of Medical Genetics, National Centre for Mitochondrial Diseases, Nice Teaching Hospital, Nice, France

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Christian Richelme MD

Christian Richelme MD

Department of Pediatrics, Nice Teaching Hospital, Nice, France

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Sabrina Sacconi MD, PhD

Sabrina Sacconi MD, PhD

National Centre for Neuromuscular Disorders, Nice Teaching Hospital, Nice, France

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Veronique Paquis-Flucklinger MD, PhD

Corresponding Author

Veronique Paquis-Flucklinger MD, PhD

Nice Sophia Antipolis University, Institute for Research on Cancer and Aging (IRCAN), CNRS, INSERM, UMR 7284 and U1081, School of Medicine, 28 avenue de Valombrose, 06107 Nice cedex 2, France

Department of Medical Genetics, National Centre for Mitochondrial Diseases, Nice Teaching Hospital, Nice, France

Correspondence to: V. Paquis-Flucklinger; e-mail: [email protected]Search for more papers by this author
First published: 20 July 2016
https://doi.org/10.1002/mus.25262
Citations: 5

ABSTRACT

Introduction: Acyl-coenzyme A dehydrogenase 9 (ACAD9) has a role in mitochondrial complex I (CI) assembly. Only a few patients who carry ACAD9 mutations have been reported. They mainly present with severe hypertrophic cardiomyopathy, although a minority have only mild isolated myopathy. Although the secondary factors influencing disease severity have not been elucidated, conservation of CI assembly and residual enzymatic activity have been suggested as explanations for the mild phenotypes associated with ACAD9 mutations. Methods: We report a novel homozygous ACAD9 mutation (c.1240C>T; p.Arg414Cys) in a 34-year-old woman who presented with non-progressive myopathy. Results: We show that this ACAD9 mutation led to a severe defect in CI assembly in the patient's muscle. Furthermore, the impact of CI deficiency is confirmed by accumulation of mitochondrial DNA deletions. Conclusion: Our data suggest that a major defect of CI assembly is not responsible for a severe phenotype. Muscle Nerve 55: 919–922, 2017

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