Exome sequencing identifies ACAD9 mutations as a cause of complex I deficiency |
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| Authors: | Haack Tobias B Danhauser Katharina Haberberger Birgit Hoser Jonathan Strecker Valentina Boehm Detlef Uziel Graziella Lamantea Eleonora Invernizzi Federica Poulton Joanna Rolinski Boris Iuso Arcangela Biskup Saskia Schmidt Thorsten Mewes Hans-Werner Wittig Ilka Meitinger Thomas Zeviani Massimo Prokisch Holger |
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| Affiliation: | Institute of Human Genetics, Helmholtz Zentrum München, German Research Center for Environmental Health, Neuherberg, Germany. |
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| Abstract: | An isolated defect of respiratory chain complex I activity is a frequent biochemical abnormality in mitochondrial disorders. Despite intensive investigation in recent years, in most instances, the molecular basis underpinning complex I defects remains unknown. We report whole-exome sequencing of a single individual with severe, isolated complex I deficiency. This analysis, followed by filtering with a prioritization of mitochondrial proteins, led us to identify compound heterozygous mutations in ACAD9, which encodes a poorly understood member of the mitochondrial acyl-CoA dehydrogenase protein family. We demonstrated the pathogenic role of the ACAD9 variants by the correction of the complex I defect on expression of the wildtype ACAD9 protein in fibroblasts derived from affected individuals. ACAD9 screening of 120 additional complex I-defective index cases led us to identify two additional unrelated cases and a total of five pathogenic ACAD9 alleles. |
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