Molecular diagnosis in mitochondrial complex I deficiency using exome sequencing. Issue 4 (12th April 2012)

Record Type:: Journal Article
Title:: Molecular diagnosis in mitochondrial complex I deficiency using exome sequencing. Issue 4 (12th April 2012)
Main Title:: Molecular diagnosis in mitochondrial complex I deficiency using exome sequencing
Authors:: Haack, Tobias B
Haberberger, Birgit
Frisch, Eva-Maria
Wieland, Thomas
Iuso, Arcangela
Gorza, Matteo
Strecker, Valentina
Graf, Elisabeth
Mayr, Johannes A
Herberg, Ulrike
Hennermann, Julia B
Klopstock, Thomas
Kuhn, Klaus A
Ahting, Uwe
Sperl, Wolfgang
Wilichowski, Ekkehard
Hoffmann, Georg F
Tesarova, Marketa
Hansikova, Hana
Zeman, Jiri
Plecko, Barbara
Zeviani, Massimo
Wittig, Ilka
Strom, Tim M
Schuelke, Markus
Freisinger, Peter
Meitinger, Thomas
Prokisch, Holger
Abstract:: Abstract : Background: Next generation sequencing has become the core technology for gene discovery in rare inherited disorders. However, the interpretation of the numerous sequence variants identified remains challenging. We assessed the application of exome sequencing for diagnostics in complex I deficiency, a disease with vast genetic heterogeneity. Methods: Ten unrelated individuals with complex I deficiency were selected for exome sequencing and sequential bioinformatic filtering. Cellular rescue experiments were performed to verify pathogenicity of novel disease alleles. Results: The first filter criterion was 'Presence of known pathogenic complex I deficiency variants'. This revealed homozygous mutations in NDUFS3 and ACAD9 in two individuals. A second criterion was 'Presence of two novel potentially pathogenic variants in a structural gene of complex I', which discovered rare variants in NDUFS8 in two unrelated individuals and in NDUFB3 in a third. Expression of wild-type cDNA in mutant cell lines rescued complex I activity and assembly, thus providing a functional validation of their pathogenicity. Using the third criterion 'Presence of two potentially pathogenic variants in a gene encoding a mitochondrial protein', loss-of-function mutations in MTFMT were discovered in two patients. In three patients the molecular genetic correlate remained unclear and follow-up analysis is ongoing. Conclusion: Appropriate in silico filtering of exome sequencing data, coupled with … (more)
Is Part Of:: Journal of medical genetics. Volume 49:Issue 4(2012)
Journal:: Journal of medical genetics
Issue:: Volume 49:Issue 4(2012)
Issue Display:: Volume 49, Issue 4 (2012)
Year:: 2012
Volume:: 49
Issue:: 4
Issue Sort Value:: 2012-0049-0004-0000
Page Start:: 277
Page End:: 283
Publication Date:: 2012-04-12
Subjects:: Exome sequencing -- mitochondrial complex I deficiency -- NDUFB3 -- MTFMT
Medical genetics -- Periodicals
616.042
Journal URLs:: http://jmg.bmjjournals.com/ ↗
http://www.bmj.com/archive ↗
DOI:: 10.1136/jmedgenet-2012-100846 ↗
Languages:: English
ISSNs:: 1468-6244
Deposit Type:: Legaldeposit
View Content:: Available online (eLD content is only available in our Reading Rooms) ↗
Physical Locations:: British Library DSC - BLDSS-3PM
British Library HMNTS - ELD Digital store
Ingest File:: 18754.xml