Přístupnostní navigace
E-přihláška
Vyhledávání Vyhledat Zavřít
Detail publikace
SÝNKOVÁ, I. BÉBAROVÁ, M. ANDRŠOVÁ, I. CHMELÍKOVÁ, L. ŠVECOVÁ, O. HOŠEK, J. PÁSEK, M. VÍT, P. VALÁŠKOVÁ, I. GAILLYOVÁ, R. NAVRÁTIL, R. NOVOTNÝ, T.
Originální název
Long-QT founder variant T309I-Kv7.1 with dominant negative pattern may predispose delayed afterdepolarizations under β-adrenergic stimulation
Typ
článek v časopise ve Web of Science, Jimp
Jazyk
angličtina
Originální abstrakt
The variant c.926C > T (p.T309I) in KCNQ1 gene was identified in 10 putatively unrelated Czech families with long QT syndrome (LQTS). Mutation carriers (24 heterozygous individuals) were more symptomatic compared to their non-affected relatives (17 individuals). The carriers showed a mild LQTS phenotype including a longer QTc interval at rest (466 ± 24 ms vs. 418 ± 20 ms) and after exercise (508 ± 32 ms vs. 417 ± 24 ms), 4 syncopes and 2 aborted cardiac arrests. The same haplotype associated with the c.926C > T variant was identified in all probands. Using the whole cell patch clamp technique and confocal microscopy, a complete loss of channel function was revealed in the homozygous setting, caused by an impaired channel trafficking. Dominant negativity with preserved reactivity to β-adrenergic stimulation was apparent in the heterozygous setting. In simulations on a human ventricular cell model, the dysfunction resulted in delayed afterdepolarizations (DADs) and premature action potentials under β-adrenergic stimulation that could be prevented by a slight inhibition of calcium current. We conclude that the KCNQ1 variant c.926C > T is the first identified LQTS-related founder mutation in Central Europe. The dominant negative channel dysfunction may lead to DADs under β-adrenergic stimulation. Inhibition of calcium current could be possible therapeutic strategy in LQTS1 patients refractory to β-blocker therapy.
Klíčová slova
long QT syndrome, KCNQ1, mutation, founder, dominant negative, delayed 30 afterdepolarization
Autoři
SÝNKOVÁ, I.; BÉBAROVÁ, M.; ANDRŠOVÁ, I.; CHMELÍKOVÁ, L.; ŠVECOVÁ, O.; HOŠEK, J.; PÁSEK, M.; VÍT, P.; VALÁŠKOVÁ, I.; GAILLYOVÁ, R.; NAVRÁTIL, R.; NOVOTNÝ, T.
Vydáno
11. 2. 2021
Nakladatel
Nature
Místo
Spojené království Velké Británie a Severního Irska
ISSN
2045-2322
Periodikum
Scientific Reports
Ročník
11
Číslo
1
Stát
Strany od
Strany do
13
Strany počet
URL
https://www.nature.com/articles/s41598-021-81670-1#Ack1
Plný text v Digitální knihovně
http://hdl.handle.net/11012/202247
BibTex
@article{BUT171501, author="Iva {Sýnková} and Markéta {Bébarová} and Irena {Andršová} and Larisa {Chmelíková} and Olga {Švecová} and Jan {Hošek} and Michal {Pásek} and Pavel {Vít} and Iveta {Valášková} and Renata {Gaillyová} and Rostislav {Navrátil} and Tomáš {Novotný}", title="Long-QT founder variant T309I-Kv7.1 with dominant negative pattern may predispose delayed afterdepolarizations under β-adrenergic stimulation", journal="Scientific Reports", year="2021", volume="11", number="1", pages="1--13", doi="10.1038/s41598-021-81670-1", issn="2045-2322", url="https://www.nature.com/articles/s41598-021-81670-1#Ack1" }