Arrhythmogenic Biophysical Phenotype for SCN5A Mutation S1787N Depends upon Splice Variant Background and Intracellular Acidosis

Hu, Rou Mu; Tan, Bi Hua; Tester, David J.; Song, Chunhua; He, Yang; Dovat, Sinisa; Peterson, Blaise Z.; Ackerman, Michael J.; Makielski, Jonathan C.

doi:10.1371/journal.pone.0124921

Cited by 16 publications

(11 citation statements)

References 43 publications

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“…When compared with non-failing adult human heart, there were no differences in total SCN5A , SCN5A-6 , or SCN5A-6A expression ( Figure S3 B). We also investigated several common polymorphisms in SCN5A that are known to result in gain or loss of function, depending on the presence of other genetic mutations ( Ackerman et al., 2004 , Cheng et al., 2011 , Hu et al., 2015 , Kapplinger et al., 2015 , Makielski et al., 2003 , Shinlapawittayatorn et al., 2011 , Ye et al., 2003 ). We tested the four most likely polymorphisms S524Y, H558R, 1077del, or R1193Q.…”

Section: Resultsmentioning

confidence: 99%

Channelopathy as a SUDEP Biomarker in Dravet Syndrome Patient-Derived Cardiac Myocytes

et al. 2018

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SummaryDravet syndrome (DS) is a severe developmental and epileptic encephalopathy with a high incidence of sudden unexpected death in epilepsy (SUDEP). Most DS patients carry de novo variants in SCN1A, resulting in Nav1.1 haploinsufficiency. Because SCN1A is expressed in heart and in brain, we proposed that cardiac arrhythmia contributes to SUDEP in DS. We generated DS patient and control induced pluripotent stem cell-derived cardiac myocytes (iPSC-CMs). We observed increased sodium current (INa) and spontaneous contraction rates in DS patient iPSC-CMs versus controls. For the subject with the largest increase in INa, cardiac abnormalities were revealed upon clinical evaluation. Generation of a CRISPR gene-edited heterozygous SCN1A deletion in control iPSCs increased INa density in iPSC-CMs similar to that seen in patient cells. Thus, the high risk of SUDEP in DS may result from a predisposition to cardiac arrhythmias in addition to seizures, reflecting expression of SCN1A in heart and brain.

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Section: Resultsmentioning

confidence: 99%

Channelopathy as a SUDEP Biomarker in Dravet Syndrome Patient-Derived Cardiac Myocytes

et al. 2018

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“…The dramatic increased late I Na found for SCN5A-N406K is typical of LQT3 [20]. The persistent Na current during action potential plateau is due to the failure of fast Na channel inactivation [8].…”

Section: Discussionmentioning

confidence: 99%

Mexiletine rescues a mixed biophysical phenotype of the cardiac sodium channel arising from the SCN5A mutation, N406K, found in LQT3 patients

Tester

et al. 2018

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Introduction: Individual mutations in the SCN5A-encoding cardiac sodium channel α-subunit usually cause a single cardiac arrhythmia disorder, some cause mixed biophysical or clinical phenotypes. Here we report an infant, female patient harboring a N406K mutation in SCN5A with a marked and mixed biophysical phenotype and assess pathogenic mechanisms. Methods and Results: A patient suffered from recurrent seizures during sleep and torsades de pointes with a QTc of 530 ms. Mutational analysis identified a N406K mutation in SCN5A. The mutation was engineered by site-directed mutagenesis and heterologously expressed in HEK293 cells. After 48 hours incubation with and without mexiletine, macroscopic voltage-gated sodium current (INa) was measured with standard whole-cell patch clamp techniques. SCN5A-N406K elicited both a significantly decreased peak INa and a significantly increased late INa compared to wide-type (WT) channels. Furthermore, mexiletine both restored the decreased peak INa of the mutant channel and inhibited the increased late INa of the mutant channel. Conclusion: SCN5A-N406K channel displays both “gain-of-function” in late INa and “loss-of-function” in peak INa density contributing to a mixed biophysical phenotype. Moreover, our finding may provide the first example that mexiletine exerts a dual rescue of both “gain-of-function” and “loss-of-function” of the mutant sodium channel.

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“…109 Other groups have shown that certain long QT type 3 syndrome mutations are more sensitive to intracellular acidosis than others. 111 Another environmental factor modulating the Na C channel is body temperature. In healthy humans, without underlying mutations in Na v 1.5 or other conditions, temperature-dependent cardiac abnormalities may occur in extreme hyperthermia but seldom when they experience a mild fever.…”

Section: Environmental Regulation Of Inactivationmentioning

confidence: 99%

Mechanisms and models of cardiac sodium channel inactivation

et al. 2017

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Shortly after cardiac Na channels activate and initiate the action potential, inactivation ensues within milliseconds, attenuating the peak Na current, I and allowing the cell membrane to repolarize. A very limited number of Na channels that do not inactivate carry a persistent I, or late I. While late I is only a small fraction of peak magnitude, it significantly prolongs ventricular action potential duration, which predisposes patients to arrhythmia. Here, we review our current understanding of inactivation mechanisms, their regulation, and how they have been modeled computationally. Based on this body of work, we conclude that inactivation and its connection to late I would be best modeled with a "feet-on-the-door" approach where multiple channel components participate in determining inactivation and late I. This model reflects experimental findings showing that perturbation of many channel locations can destabilize inactivation and cause pathological late I.

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Arrhythmogenic Biophysical Phenotype for SCN5A Mutation S1787N Depends upon Splice Variant Background and Intracellular Acidosis

Cited by 16 publications

References 43 publications

Channelopathy as a SUDEP Biomarker in Dravet Syndrome Patient-Derived Cardiac Myocytes

Channelopathy as a SUDEP Biomarker in Dravet Syndrome Patient-Derived Cardiac Myocytes

Mexiletine rescues a mixed biophysical phenotype of the cardiac sodium channel arising from the SCN5A mutation, N406K, found in LQT3 patients

Mechanisms and models of cardiac sodium channel inactivation

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