Combination of cardiac conduction disease and long QT syndrome caused by mutation T1620K in the cardiac sodium channel

doi:10.1093/cvr/cvm096

Cardiovascular Research Advance Access [Accepted Manuscript] published online on December 7, 2007
Cardiovascular Research, doi:10.1093/cvr/cvm096

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Combination of cardiac conduction disease and long QT syndrome caused by mutation T1620K in the cardiac sodium channel

Ralf Surber^*^,1, Sabine Hensellek^*^,2, Dirk Prochnau¹, Gerald S. Werner¹, Klaus Benndorf², Hans R. Figulla¹ and Thomas Zimmer²

¹ Department of Internal Medicine I
² Institute of Physiology II Friedrich Schiller University Jena, 07740 Jena, Germany

Corresponding author: Thomas Zimmer, Ph.D. , Institute of Physiology II, Friedrich Schiller University Jena, Kollegiengasse 9, 07743 Jena, Germany. Tel.: +49-3641-934372, FAX: +49-3641-933202, Email: thomas.zimmer{at}mti.uni-jena.de

Aims: The aim of the present study was to elucidate the molecularmechanism underlying the concomitant occurrence of cardiac conductiondisease (CCD) and long QT syndrome (LQT3), two SCN5A channelopathiesthat are explained by loss-of-function and gain-of-function,respectively, in the cardiac Na⁺ channel.

Methods: A Caucasian family with prolonged QT interval, intermittentbundle-branch block, sudden cardiac death and syncope was investigated.Lidocaine (1 mg/kg i.v.) normalized the prolonged QT intervaland rescued bundle-branch block. An SCN5A mutation analysiswas performed that revealed a C-to-A mutation at position 4859(exon 28), predicted to change a highly conserved threoninefor a lysine at position 1620. Mutant channels were characterizedboth in Xenopus oocytes and HEK293 cells.

Results: The T1620K mutation remarkably altered the properties of Na_v1.5channels. In particular, the voltage-dependence of the currentdecay time constants was largely lost. As a consequence, mutantchannels inactivated faster than wild-type channels at potentialsnegative to -30 mV, resulting in less Na⁺ inward current (loss-of-function),but significantly slower at potentials positive to -30 mV, resultingin an increased Na⁺ inward current (gain-of-function). Moreover,we found a hyperpolarized shift of steady-state activation andan accelerated recovery from inactivation (gain-of-function).At the same time, channel availability was significantly reducedat the resting membrane potential (loss-of-function).

Conclusion: We conclude that lysine at position 1620 leads to both loss-of-functionand gain-of-function properties in hNa_v1.5 channels, which mayconsequently cause in the same individuals impaired impulsepropagation in the conduction system and prolonged QTc intervals,respectively.

Time for primary review: 21

^* These authors contributed equally to this work.

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