Mutations in Danish patients with long QT syndrome and the identification of a large founder family with p.F29L in KCNH2

Christiansen, Michael; Hedley, Paula L.; Theilade, Juliane; Stoevring, Birgitte; Leren, Trond P.; Eschen, Ole; Sørensen, Karina M.; Tybjærg-Hansen, Anne; Ousager, Lilian B.; Pedersen, Lisbeth N.; Frikke-Schmidt, Ruth; Aidt, Frederik H.; Hansen, Michael G.; Hansen, Jim; Bloch Thomsen, Poul E.; Toft, Egon; Henriksen, Finn L.; Bundgaard, Henning; Jensen, Henrik K.; Kanters, Jorgen K.

Mutations in Danish patients with long QT syndrome and the identification of a large founder family with p.F29L in KCNH2

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Date

2014-03

Authors

Christiansen, Michael

Hedley, Paula L.

Theilade, Juliane

Stoevring, Birgitte

Leren, Trond P.

Eschen, Ole

Sørensen, Karina M.

Tybjærg-Hansen, Anne

Ousager, Lilian B.

Pedersen, Lisbeth N.

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Publisher

BioMed Central

Abstract

Background: Long QT syndrome (LQTS) is a cardiac ion channelopathy which presents clinically with palpitations, syncope or sudden death. More than 700 LQTS-causing mutations have been identified in 13 genes, all of which encode proteins involved in the execution of the cardiac action potential. The most frequently affected genes, covering > 90% of cases, are KCNQ1, KCNH2 and SCN5A. Methods: We describe 64 different mutations in 70 unrelated Danish families using a routine five-gene screen, comprising KCNQ1, KCNH2 and SCN5A as well as KCNE1 and KCNE2. Results: Twenty-two mutations were found in KCNQ1, 28 in KCNH2, 9 in SCN5A, 3 in KCNE1 and 2 in KCNE2. Twenty-six of these have only been described in the Danish population and 18 are novel. One double heterozygote (1.4% of families) was found. A founder mutation, p.F29L in KCNH2, was identified in 5 “unrelated” families. Disease association, in 31.2% of cases, was based on the type of mutation identified (nonsense, insertion/deletion, frameshift or splice-site). Functional data was available for 22.7% of the missense mutations. None of the mutations were found in 364 Danish alleles and only three, all functionally characterised, were recorded in the Exome Variation Server, albeit at a frequency of < 1:1000. Conclusion: The genetic etiology of LQTS in Denmark is similar to that found in other populations. A large founder family with p.F29L in KCNH2 was identified. In 48.4% of the mutations disease causation was based on mutation type or functional analysis.

Description

Please cite as follows: Christiansen, M. et al. 2014. Mutations in Danish patients with long QT syndrome and the identification of a large founder family with p.F29L in KCNH2. BMC Medical Genetics, 15(1):31, doi:10.1186/1471-2350-15-31.
The original publication is available at http://www.biomedcentral.com/1471-2350/15/31

Keywords

Long QT syndrome, Heart -- Ventricles -- Abnormalities, Long QT syndrome -- Genetic aspects

Citation

Christiansen, M. et al. 2014. Mutations in Danish patients with long QT syndrome and the identification of a large founder family with p.F29L in KCNH2. BMC Medical Genetics, 15(1):31, doi:10.1186/1471-2350-15-31.

URI

http://hdl.handle.net/10019.1/95561

Collections

Research Articles (Molecular Biology and Human Genetics)

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