A novel NaV1.5 voltage sensor mutation associated with severe atrial and ventricular arrhythmias

Wang, Honggang; Zhu, Wandi; Kanter, Ronald J.; Silva, Jonathan R.; Honeywell, Christina; Gow, Robert M.; Pitt, Geoffrey S.

doi:10.1016/j.yjmcc.2016.01.014

Cited by 22 publications

(22 citation statements)

References 38 publications

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“…Those results were basically consistent with previous studies (16,17). As for R965C-R1309H mutations, compared to R1309H mutation, it induced more significant depolarization shift of activation curve, V 1/2 and slope factor, suggesting that Na v 1.5 R965C-R1309H channel was activated at the much more depolarized membrane potential and displayed slower activation (Supplement 3).…”

Section: Electrophysiological Characteristicssupporting

confidence: 92%

“…Consistent with previous literatures reported (16,17), as shown in the Figure 4A-C and Table 2, the R1309H mutation, but not R965C mutation, significantly reduced the Na + current density at a series of test potentials ranging from -45 mV to -15 mV when compared to the WT group (Supplement 1). More importantly, we found that R965C-R1309H mutations resulted in a more severe reduction in Na + current density ranging from -45 mV to 30 mV compared to the WT group.…”

Section: Electrophysiological Characteristicssupporting

confidence: 91%

“…And the slope factor (K) of R1309H mutation was significant amplified but not of R965C mutation when compared to the WT group. These above data were keeping with the previous studies (16,17). We were surprised to find that the inactivation curve of R965C-R1309H mutations most significantly shifted to the left with the increase of V 1/2 hyperpolarization and K value ( Figure 5C, Table 3).…”

Section: Electrophysiological Characteristicssupporting

confidence: 90%

“…The R1309H mutation significantly reduced the current density of I Na , hyperpolarized inactivation, slowed recovery from inactivation, and increased the I NaL. It was noted that the carriers with heterozygous R1309H mutation showed slightly abnormal ECGs without arrhythmia events (16).…”

Section: Compound Mutations Of R965c and R1309h Synergistically Aggramentioning

confidence: 98%

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More Severe Loss-of-Function Sodium Channel induced by Compound SCN5A R965C and R1309H Mutants lead to Complex Familial Arrhythmia Syndrome

Lin

Qin

Shen

et al. 2019

Preprint

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Objective: A complex familial arrhythmia syndrome was identified in a Chinese Han family, characterized by sick sinus syndrome, progressive conduction block, atrial fibrillation, atrial standstill and Brugada syndrome. The underlying mechanism associated with the genetic mutation was investigated. Methods: Genetic analysis was conducted for probands in the coding and splicing regions of genes susceptible to cardiac arrhythmia diseases. The stable cell lines overexpressing wild-type (WT) or mutant SCN5A gene were generated in HEK293T cells and electrophysiological recordings were performed to evaluate the functional changes of mutant Na V 1.5 channels. Results: We identified a rare double R965C and R1309H mutations in Na V 1.5 channel, as a heterozygous and compound pattern, locating in the same chromosome.Compared to WT, a single mutation of R965C or R1309H, the compound mutations of R965C-R1309H most dramatically reduced the peak current of Na V 1.5 channel with testing potentials ranging from -35 mV to 25 mV. Notably, the maximal peak current of Na V 1.5 channel carrying R1309H only and R965C-R1309H mutations displayed significant decreases by 31.5% and 73.34%, respectively, compared to WT. Additionally, compared to single mutations of R965C or R1309H, the R965C-R1309H mutations resulted in more obviously depolarization-shifted activation and hyperpolarization-shifted inactivation, also caused most significantly changed time constant, V 1/2 and slope factor of activation and inactivation. Conclusions:The compound mutations of R965C-R1309H led to more dramatically reduced current density of Na v 1.5 channel, as well as more depolarization-shifted activation and hyperpolarization-shifted inactivation than single mutation of R965C or R1309H, which may provide more understanding on the molecular mechanisms underlying the familial arrhythmia syndrome. Author summarySeveral limited types of research about the interaction of compound mutations and the mechanism of interaction remains controversial. Here we report a novel compound mutation R965C-R1309H in SCN5A gene.The compound mutations of R965C-R1309H markedly reduced the Na + current density of Na v 1.5 channel and caused significant depolarization-shifted activation and hyperpolarization-shifted inactivation, suggesting that R965C mutation aggravated the pore gating changes of sodium channel containing R1309H mutation. The R965C located in the S4-like region in the intracellular loop between DII and DIII, and the R1309H located in the S4 helix of DIII as voltage sensor, which thus potentially had synergistic and interacting effects on pore gating properties of the sodium channel. Additionally, the complex familial arrhythmia syndrome simultaneously complicated of early young onset of arrhythmia and harmful prognosis of recurrent ischemic cerebral stroke, even though effective Warfarin anticoagulation. overlap syndrome, heritable/familial arrhythmia syndrome or SCN5A syndrome induced by a single or several SCN5A mutations.Here, we report a Han Chinese family presen...

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Section: Electrophysiological Characteristicssupporting

confidence: 92%

Section: Electrophysiological Characteristicssupporting

confidence: 91%

Section: Electrophysiological Characteristicssupporting

confidence: 90%

Section: Compound Mutations Of R965c and R1309h Synergistically Aggramentioning

confidence: 98%

See 2 more Smart Citations

More Severe Loss-of-Function Sodium Channel induced by Compound SCN5A R965C and R1309H Mutants lead to Complex Familial Arrhythmia Syndrome

Lin

Qin

Shen

et al. 2019

Preprint

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“…Ion channels represent a family of important membrane proteins that conduct ions across the membrane, thereby controlling the intracellular ion content, membrane potential and action potentials. The abnormal function and structure of ion channels can lead to a variety of cardiovascular diseases (Ackerman, ; Navedo et al, ; Hsiao et al, ; George, ; Wang et al, ). More importantly, endogenous sulfur‐containing gaseous signal molecules play an important role in the pathogenesis of cardiovascular diseases by targeting ion channels (Wang, ; Brampton and Aaronson, ).…”

Section: Introductionmentioning

confidence: 99%

Sulfur‐containing gaseous signal molecules, ion channels and cardiovascular diseases

Wen

Jin

Tang

et al. 2017

British J Pharmacology

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Identification of rare heterozygous linkage R965C‐R1309H mutations in the pore‐forming region of SCN5A gene associated with complex arrhythmia

Lin

Qin

Shen

et al. 2021

Molec Gen & Gen Med

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A novel NaV1.5 voltage sensor mutation associated with severe atrial and ventricular arrhythmias

Cited by 22 publications

References 38 publications

More Severe Loss-of-Function Sodium Channel induced by Compound SCN5A R965C and R1309H Mutants lead to Complex Familial Arrhythmia Syndrome

More Severe Loss-of-Function Sodium Channel induced by Compound SCN5A R965C and R1309H Mutants lead to Complex Familial Arrhythmia Syndrome

Sulfur‐containing gaseous signal molecules, ion channels and cardiovascular diseases

Identification of rare heterozygous linkage R965C‐R1309H mutations in the pore‐forming region of SCN5A gene associated with complex arrhythmia

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