Facilitation of <i>I</i>Kr current by some hERG channel blockers suppresses early afterdepolarizations

Furutani, Kazuharu; Tsumoto, Kunichika; Chen, I‐Shan; Handa, Kenichiro; Yamakawa, Yuko; Sack, Jon T.; Kurachi, Yoshihisa

doi:10.1085/jgp.201812192

Cited by 20 publications

(40 citation statements)

References 72 publications

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“…2Aa,Ba, red line). Reducing the %g Na,LM by 65%, corresponding to , and pre-junctional membrane (pre-JM) segments, and each membrane segment comprises a modified O'Hara-Rudy dynamic (mORd) ventricular myocyte model [10][11][12] and membrane capacitance, C m,l , for l = post-JM, LM, and pre-JM (c). In (d), V k j represents extracellular cleft potential just after the kth myocyte.…”

Section: Resultsmentioning

confidence: 99%

“…Allocating Na + channel conductances to each membrane segment and changing those individually, we altered the subcellular expression of Na + channels. The electrophysiological property of each membrane segment was represented by a modified O'Hara-Rudy dynamic (mORd) model 10,11 , which is the most sophisticated human ventricular AP model to date that extensively validated against experimental data from more than 100 non-diseased human hearts. For better correspondence with the experimental CV of human RV epicardium 52 , the formula of fast I Na in the O'Hara-Rudy dynamic model was replaced with that of the ten Tusscher-Panfilov (TP) model 12 .…”

Section: Methodsmentioning

confidence: 99%

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Specific decreasing of Na+ channel expression on the lateral membrane of cardiomyocytes causes fatal arrhythmias in Brugada syndrome

Tsumoto

Ashihara

Naito

et al. 2020

Sci Rep

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Reduced cardiac sodium (Na+) channel current (INa) resulting from the loss-of-function of Na+ channel is a major cause of lethal arrhythmias in Brugada syndrome (BrS). Inspired by previous experimental studies which showed that in heart diseases INa was reduced along with expression changes in Na+ channel within myocytes, we hypothesized that the local decrease in INa caused by the alteration in Na+ channel expression in myocytes leads to the occurrence of phase-2 reentry, the major triggering mechanism of lethal arrhythmias in BrS. We constructed in silico human ventricular myocardial strand and ring models, and examined whether the Na+ channel expression changes in each myocyte cause the phase-2 reentry in BrS. Reducing Na+ channel expression in the lateral membrane of each myocyte caused not only the notch-and-dome but also loss-of-dome type action potentials and slowed conduction, both of which are typically observed in BrS patients. Furthermore, the selective reduction in Na+ channels on the lateral membrane of each myocyte together with spatial tissue heterogeneity of Na+ channel expression caused the phase-2 reentry and phase-2 reentry-mediated reentrant arrhythmias. Our data suggest that the BrS phenotype is strongly influenced by expression abnormalities as well as genetic abnormalities of Na+ channels.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Specific decreasing of Na+ channel expression on the lateral membrane of cardiomyocytes causes fatal arrhythmias in Brugada syndrome

Tsumoto

Ashihara

Naito

et al. 2020

Sci Rep

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“…The latter equation is similar to the equation obtained in this study. Another study performed by K. Furutani et al [43] discusses a model for I K . K. Furutani et al [43] mention two equations that model the activation and inactivation of the I K channels and both equations have exponential expressions on them.…”

Section: Plos Onementioning

confidence: 99%

Model based estimation of QT intervals in non-invasive fetal ECG signals

et al. 2020

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The end timing of T waves in fetal electrocardiogram (fECG) is important for the evaluation of ST and QT intervals which are vital markers to assess cardiac repolarization patterns. Monitoring malignant fetal arrhythmias in utero is fundamental to care in congenital heart anomalies preventing perinatal death. Currently, reliable detection of end of T waves is possible only by using fetal scalp ECG (fsECG) and fetal magnetocardiography (fMCG). fMCG is expensive and less accessible and fsECG is an invasive technique available only during intrapartum period. Another safer and affordable alternative is the non-invasive fECG (nfECG) which can provide similar assessment provided by fsECG and fMECG but with less accuracy (not beat by beat). Detection of T waves using nfECG is challenging because of their low amplitudes and high noise. In this study, a novel model-based method that estimates the end of T waves in nfECG signals is proposed. The repolarization phase has been modeled as the discharging phase of a capacitor. To test the model, fECG signals were collected from 58 pregnant women (age: (34 ± 6) years old) bearing normal and abnormal fetuses with gestational age (GA) 20-41 weeks. QT and QTc intervals have been calculated to test the level of agreement between the model-based and reference values (fsECG and Doppler Ultrasound (DUS) signals) in normal subjects. The results of the test showed high agreement between modelbased and reference values (difference < 5%), which implies that the proposed model could be an alternative method to detect the end of T waves in nfECG signals.

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“…Allocating Na + channel conductances to each membrane segment and changing those individually, we altered the subcellular expression of Na + channels. The electrophysiological property of each membrane segment was represented by the O'Hara-Rudy dynamic (ORd) model (16,17), which is the most sophisticated human ventricular AP model to date that extensively validated against experimental data from more than 100 non-diseased human hearts. For better correspondence with the experimental conduction velocity of human RV epicardium (18), the formula of fast I Na in the ORd model was replaced with that of the ten Tusscher-Panfilov (TP) model (19).…”

Section: Myocardial Strand and Ring Models And Subcellular Na + Channmentioning

confidence: 99%

“…Electrophysiological properties of each membrane segment composing the ventricular myocyte were described by a modified O'Hara-Rudy dynamic (mORd) model (16). The mORd model consisted of a membrane capacitance and several ion channel currents, including our modification (17) to the original currents of a potassium channel (I Kr ). Furthermore, the fast I Na in the original ORd model was replaced with that of the ten Tusscher-Panfilov (TP) model (19).…”

Section: Myocardial Strand and Ring Modelsmentioning

confidence: 99%

Specific decreasing of Na⁺ channel expression on the lateral membrane of cardiomyocytes causes fatal arrhythmias in Brugada syndrome

Tsumoto

Ashihara

Naito

et al. 2019

Preprint

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Non-standard Abbreviations and Acronyms: LM: lateral membrane of cardiomyocytes; JM: junctional membrane of cardiomyocytes; pre-JM: pre-junctional membrane of cardiomyocytes; post-JM: post-junctional membrane of cardiomyocyte; I Na,LM : I Na across the LM; I Na,pre-JM : I Na across the pre-JM; I Na,post-JM : I Na across the post-JM; V m,pre-JM : membrane potential of the pre-JM; V m,post-JM : membrane potential of the post-JM 1 ABSTRACT One phenotypic feature of Brugada syndrome (BrS) is slowed conduction due to the reduction (loss-of-function) of Na + channels. In contrast, recent clinical observations in BrS patients highlighted the poor correlation between the phenotype (typical ECG change or lethal arrhythmia) and the genotype (SCN5A mutation). Inspired by our previous theoretical study which showed that reduced Na + channels in the lateral membrane (LM) of ventricular myocytes caused the slowing of conduction under myocardial ischemia, we hypothesized that a loss-of-function of Na + channels caused by the decreases in Na + channel expression within myocytes leads to phase-2 reentry (P2R), the major triggering mechanism of lethal arrhythmias in BrS. We constructed an in silico human ventricular myocardial strand and ring models, and investigated the relationship between the subcellular Na + channel distribution and P2R. Reducing Na + channel expression in the LM of each myocyte caused not only the notch-and-dome but also loss-of-dome type action potentials and slowed conduction, both of which are typically observed in BrS patients. Furthermore, we showed that both the reduction in Na + channels on the LM of each myocyte and tissue-level heterogeneity of Na + channel expression were essential for P2R as well as P2R-mediated reentrant excitation. Our data suggest that the alteration in subcellular Na + channel distribution together with a tissue-level heterogeneity of Na + channels can cause arrhythmogenesis in BrS.

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Facilitation of IKr current by some hERG channel blockers suppresses early afterdepolarizations

Cited by 20 publications

References 72 publications

Specific decreasing of Na+ channel expression on the lateral membrane of cardiomyocytes causes fatal arrhythmias in Brugada syndrome

Specific decreasing of Na+ channel expression on the lateral membrane of cardiomyocytes causes fatal arrhythmias in Brugada syndrome

Model based estimation of QT intervals in non-invasive fetal ECG signals

Specific decreasing of Na⁺ channel expression on the lateral membrane of cardiomyocytes causes fatal arrhythmias in Brugada syndrome

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