Exome sequencing identifies complex I NDUFV2 mutations as a novel cause of Leigh syndrome

Jessie M Cameron; Nevena MacKay; Annette Feigenbaum; Mark Tarnopolsky; Susan Blaser; Brian H Robinson; Andreas Schulze

doi:10.1016/j.ejpn.2015.05.002

Exome sequencing identifies complex I NDUFV2 mutations as a novel cause of Leigh syndrome

Eur J Paediatr Neurol. 2015 Sep;19(5):525-32. doi: 10.1016/j.ejpn.2015.05.002. Epub 2015 May 14.

Authors

Jessie M Cameron¹, Nevena MacKay², Annette Feigenbaum³, Mark Tarnopolsky⁴, Susan Blaser⁵, Brian H Robinson⁶, Andreas Schulze⁷

Affiliations

¹ Genetics & Genome Biology Program, Peter Gilgan Centre for Research and Learning, 686 Bay Street, Toronto, ON M5G 0A4, Canada. Electronic address: jessie.cameron@sickkids.ca.
² Department of Paediatric Laboratory Medicine, The Hospital for Sick Children, 555 University Avenue, Toronto, ON M5G 1X8, Canada.
³ Division of Clinical and Metabolic Genetics, The Hospital for Sick Children and University of Toronto, Toronto, ON M5G 1X8, Canada. Electronic address: Annette.feigenbaum@sickkids.ca.
⁴ Department of Pediatrics, McMaster University Medical Center, Hamilton, ON L8N 3Z5, Canada. Electronic address: tarnopol@mcmaster.ca.
⁵ Department of Radiology, The Hospital for Sick Children and University of Toronto, ON M5G 1X8, Canada. Electronic address: Susan.blaser@sickkids.ca.
⁶ Genetics & Genome Biology Program, Peter Gilgan Centre for Research and Learning, 686 Bay Street, Toronto, ON M5G 0A4, Canada; Department of Biochemistry, University of Toronto, Toronto, ON M5S 1A8, Canada. Electronic address: Brian.robinson@sickkids.ca.
⁷ Genetics & Genome Biology Program, Peter Gilgan Centre for Research and Learning, 686 Bay Street, Toronto, ON M5G 0A4, Canada; Division of Clinical and Metabolic Genetics, The Hospital for Sick Children and University of Toronto, Toronto, ON M5G 1X8, Canada. Electronic address: Andreas.schulze@sickkids.ca.

PMID: 26008862
DOI: 10.1016/j.ejpn.2015.05.002

Abstract

Background: Two siblings with hypertrophic cardiomyopathy and brain atrophy were diagnosed with Complex I deficiency based on low enzyme activity in muscle and high lactate/pyruvate ratio in fibroblasts.

Methods: Whole exome sequencing results of fibroblast gDNA from one sibling was narrowed down to 190 SNPs or In/Dels in 185 candidate genes by selecting non-synonymous coding sequence base pair changes that were not present in the SNP database.

Results: Two compound heterozygous mutations were identified in both siblings in NDUFV2, encoding the 24 kDa subunit of Complex I. The intronic mutation (c.IVS2 + 1delGTAA) is disease causing and has been reported before. The other mutation is novel (c.669_670insG, p.Ser224Valfs*3) and predicted to cause a pathogenic frameshift in the protein. Subsequent investigation of 10 probands with complex I deficiency from different families revealed homozygosity for the intronic c.IVS2 + 1delGTAA mutation in a second, consanguineous family. In this family three of five siblings were affected. Interestingly, they presented with Leigh syndrome but no cardiac involvement. The same genotype had been reported previously in a two families but presenting with hypertrophic cardiomyopathy, trunk hypotonia and encephalopathy.

Conclusion: We have identified NDUFV2 mutations in two families with Complex I deficiency, including a novel mutation. The diagnosis of Leigh syndrome expands the clinical phenotypes associated with the c.IVS2 + 1delGTAA mutation in this gene.

Keywords: Complex I; Exome sequencing; Leigh syndrome; Mitochondria; NDUFV2.

Publication types

Case Reports
Research Support, Non-U.S. Gov't

MeSH terms

Exome* / genetics
Female
Humans
Leigh Disease / genetics*
Mutation*
NADH Dehydrogenase / genetics*
Pedigree
Phenotype
Siblings

Substances

NADH Dehydrogenase
NDUFV2 protein, human