Complex interactions in a novel SCN5A compound mutation associated with long QT and Brugada syndrome: Implications for Na(+) channel blocking pharmacotherapy for de novo conduction disease

BACKGROUND: The SCN5A mutation, P1332L, is linked to a malignant form of congenital long QT syndrome, type 3 (LQT3), and affected patients are highly responsive to the Na(+) channel blocking drug, mexiletine. In contrast, A647D is an atypical SCN5A mutation causing Brugada syndrome. An asymptomatic...

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Detalles Bibliográficos
Autores principales: Liu, Jie, Bayer, Jason D., Aschar-Sobbi, Roozbeh, Wauchop, Marianne, Spears, Danna, Gollob, Michael, Vigmond, Edward J., Tsushima, Robert, Backx, Peter H., Chauhan, Vijay S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5965851/
https://www.ncbi.nlm.nih.gov/pubmed/29791480
http://dx.doi.org/10.1371/journal.pone.0197273
Descripción
Sumario:BACKGROUND: The SCN5A mutation, P1332L, is linked to a malignant form of congenital long QT syndrome, type 3 (LQT3), and affected patients are highly responsive to the Na(+) channel blocking drug, mexiletine. In contrast, A647D is an atypical SCN5A mutation causing Brugada syndrome. An asymptomatic male with both P1332L and A647D presented with varying P wave/QRS aberrancy and mild QTc prolongation which did not shorten measurably with mexiletine. OBJECTIVE: We characterized the biophysical properties of P1332L, A647D and wild-type (WT) Na(+) channels as well as their combinations in order to understand our proband’s phenotype and to guide mexilitine therapy. METHODS: Na(+) channel biophysics and mexilitine-binding kinetics were assessed using heterologous expression studies in CHO-K1 cells and human ventricular myocyte modeling. RESULTS: Compared to WT, P1332L channels displayed a hyperpolarizing shift in inactivation, slower inactivation and prominent late Na(+) currents (I(Na)). While A647D had no effect on the biophysical properties of I(Na), it reduced peak and late I(Na) density when co-expressed with either WT or P1332L. Additionally, while P1332L channels had greater sensitivity to block by mexiletine compared to WT, this was reduced in the presence of A647D. Modelling studies revealed that mixing P1332L with A647D channels, action potential durations were shortened compared to P1332L, while peak I(Na) was reduced compared to either A647D coexpressing with WT or WT alone. CONCLUSIONS: While A647D mitigates the lethal LQT3 phenotype seen with P1332L, it also reduces mexilitine sensitivity and decreases I(Na) density. These results explain our proband’s mild repolarization abnormality and prominent conduction defect in the atria and ventricles, but also suggest that expression of P1332L with A647D yields a novel disease phenotype for which mexiletine pharmacotherapy is no longer suitable.

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