Journal
CIRCULATION-CARDIOVASCULAR GENETICS
Volume 9, Issue 5, Pages 426-435Publisher
LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1161/CIRCGENETICS.116.001431
Keywords
cardiomyopathy; left ventricular noncompaction; missense mutation; telethonin; titin; whole genome sequencing
Funding
- British Heart Foundation [FS/12/40/29712, PG/15/113/31944]
- BHF Centre of Research Excellence, Oxford [HSRNWBY, HSRNWB11, RE/13/1/30181]
- National Institute for Health Research (NIHR) [NIHR-HCS-D13-04-006]
- NIHR Biomedical Research Centre, Oxford
- Wellcome Trust [090532/Z/09/Z]
- EU MUZIC network
- MRC
- Leducq Foundation
- British Heart Foundation [RG/15/8/31480, PG/15/113/31944, FS/12/40/29712, RG/12/16/29939] Funding Source: researchfish
- Medical Research Council [MR/J010456/1, MR/K015664/1] Funding Source: researchfish
- Wellcome Trust [201543/Z/16/Z] Funding Source: researchfish
- National Institutes of Health Research (NIHR) [NIHR-HCS-D13-04-006] Funding Source: National Institutes of Health Research (NIHR)
- MRC [MR/K015664/1, MR/J010456/1] Funding Source: UKRI
- Wellcome Trust [201543/Z/16/Z] Funding Source: Wellcome Trust
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Background High throughput next-generation sequencing techniques have made whole genome sequencing accessible in clinical practice; however, the abundance of variation in the human genomes makes the identification of a disease-causing mutation on a background of benign rare variants challenging. Methods and Results Here we combine whole genome sequencing with linkage analysis in a 3-generation family affected by cardiomyopathy with features of autosomal dominant left ventricular noncompaction cardiomyopathy. A missense mutation in the giant protein titin is the only plausible disease-causing variant that segregates with disease among the 7 surviving affected individuals, with interrogation of the entire genome excluding other potential causes. This A178D missense mutation, affecting a conserved residue in the second immunoglobulin-like domain of titin, was introduced in a bacterially expressed recombinant protein fragment and biophysically characterized in comparison to its wild-type counterpart. Multiple experiments, including size exclusion chromatography, small-angle x ray scattering, and circular dichroism spectroscopy suggest partial unfolding and domain destabilization in the presence of the mutation. Moreover, binding experiments in mammalian cells show that the mutation markedly impairs binding to the titin ligand telethonin. Conclusions Here we present genetic and functional evidence implicating the novel A178D missense mutation in titin as the cause of a highly penetrant familial cardiomyopathy with features of left ventricular noncompaction. This expands the spectrum of titin's roles in cardiomyopathies. It furthermore highlights that rare titin missense variants, currently often ignored or left uninterpreted, should be considered to be relevant for cardiomyopathies and can be identified by the approach presented here.
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