The Bradycardic Agent Ivabradine Acts as an Atypical Inhibitor of Voltage-Gated Sodium Channels

Benjamin Hackl; Peter Lukacs; Janine Ebner; Krisztina Pesti; Nicholas Haechl; Mátyás C. Földi; Elena Lilliu; Klaus Schicker; Helmut Kubista; Anna Stary-Weinzinger; Karlheinz Hilber; Arpad Mike; Hannes Todt; Xaver Koenig

doi:10.3389/fphar.2022.809802

The Bradycardic Agent Ivabradine Acts as an Atypical Inhibitor of Voltage-Gated Sodium Channels

Benjamin Hackl
, Peter Lukacs
, Janine Ebner
, Krisztina Pesti
, Nicholas Haechl
, Mátyás C. Földi
, Elena Lilliu
, Klaus Schicker
, Helmut Kubista
, Anna Stary-Weinzinger
, Karlheinz Hilber
, Arpad Mike
, Hannes Todt
, Xaver Koenig (Corresponding author)

Department of Pharmaceutical Sciences

Publications: Contribution to journal › Article › Peer Reviewed

Abstract

Background and purpose: Ivabradine is clinically administered to lower the heart rate, proposedly by inhibiting hyperpolarization-activated cyclic nucleotide-gated cation channels in the sinoatrial node. Recent evidence suggests that voltage-gated sodium channels (VGSC) are inhibited within the same concentration range. VGSCs are expressed within the sinoatrial node and throughout the conduction system of the heart. A block of these channels thus likely contributes to the established and newly raised clinical indications of ivabradine. We, therefore, investigated the pharmacological action of ivabradine on VGSCs in sufficient detail in order to gain a better understanding of the pro- and anti-arrhythmic effects associated with the administration of this drug.Experimental Approach: Ivabradine was tested on VGSCs in native cardiomyocytes isolated from mouse ventricles and the His-Purkinje system and on human Na(v)1.5 in a heterologous expression system. We investigated the mechanism of channel inhibition by determining its voltage-, frequency-, state-, and temperature-dependence, complemented by a molecular drug docking to the recent Na(v)1.5 cryoEM structure. Automated patch-clamp experiments were used to investigate ivabradine-mediated changes in Na(v)1.5 inactivation parameters and inhibition of different VGSC isoforms.Key results: Ivabradine inhibited VGSCs in a voltage- and frequency-dependent manner, but did not alter voltage-dependence of activation and fast inactivation, nor recovery from fast inactivation. Cardiac (Na(v)1.5), neuronal (Na(v)1.2), and skeletal muscle (Na(v)1.4) VGSC isoforms were inhibited by ivabradine within the same concentration range, as were sodium currents in native cardiomyocytes isolated from the ventricles and the His-Purkinje system. Molecular drug docking suggested an interaction of ivabradine with the classical local anesthetic binding site.Conclusion and Implications: Ivabradine acts as an atypical inhibitor of VGSCs. Inhibition of VGSCs likely contributes to the heart rate lowering effect of ivabradine, in particular at higher stimulation frequencies and depolarized membrane potentials, and to the observed slowing of intra-cardiac conduction. Inhibition of VGSCs in native cardiomyocytes and across channel isoforms may provide a potential basis for the anti-arrhythmic potential as observed upon administration of ivabradine.

Original language	English
Article number	809802
Number of pages	15
Journal	Frontiers in Pharmacology
Volume	13
DOIs	https://doi.org/10.3389/fphar.2022.809802
Publication status	Published - 2 May 2022

Funding

This work was funded in whole, or in part, by the Austrian Science Fund (FWF) P30234-B27 to KH, P31563-B30 and ERACVD JTC2020 I04649-B to XK, and by the Hungarian Brain Research Program (KTIA-NAP-1322014002), and the Hungary's Economic Development, and Innovation Operative Programme (GINOP-2.3.2-15-2016-00051). The current study was performed under the guiding principles of the Declaration of Helsinki and coincides with the rules of the animal welfare committee at the Medical University of Vienna. Respective ethics vote from the Austrian Federal Ministry of Education, Science and Research (BMWFW) are found under the following number: BMWFW-66.009/0175-104 WF/V/3b/2015.

Austrian Fields of Science 2012

301206 Pharmacology

Keywords

atypical inhibitor
conduction cell
ivabradine
S16257
ventricular cardiomyocyte
voltage-gated sodium channel
VENTRICULAR RATE
SINOATRIAL NODE
ATRIAL-FIBRILLATION
JUNCTIONAL ECTOPIC TACHYCARDIA
TARGETED DISRUPTION
FUNCTIONAL EXPRESSION
ATRIOVENTRICULAR-BLOCK
HEART-RATE REDUCTION
CARDIAC PREPARATIONS
I-F INHIBITION

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https://phaidra.univie.ac.at/o:1670949Licence: CC BY 4.0

Cite this

Hackl, B., Lukacs, P., Ebner, J., Pesti, K., Haechl, N., Földi, M. C., Lilliu, E., Schicker, K., Kubista, H., Stary-Weinzinger, A., Hilber, K., Mike, A., Todt, H., & Koenig, X. (2022). The Bradycardic Agent Ivabradine Acts as an Atypical Inhibitor of Voltage-Gated Sodium Channels. Frontiers in Pharmacology, 13, Article 809802. https://doi.org/10.3389/fphar.2022.809802

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title = "The Bradycardic Agent Ivabradine Acts as an Atypical Inhibitor of Voltage-Gated Sodium Channels",

abstract = "Background and purpose: Ivabradine is clinically administered to lower the heart rate, proposedly by inhibiting hyperpolarization-activated cyclic nucleotide-gated cation channels in the sinoatrial node. Recent evidence suggests that voltage-gated sodium channels (VGSC) are inhibited within the same concentration range. VGSCs are expressed within the sinoatrial node and throughout the conduction system of the heart. A block of these channels thus likely contributes to the established and newly raised clinical indications of ivabradine. We, therefore, investigated the pharmacological action of ivabradine on VGSCs in sufficient detail in order to gain a better understanding of the pro- and anti-arrhythmic effects associated with the administration of this drug.Experimental Approach: Ivabradine was tested on VGSCs in native cardiomyocytes isolated from mouse ventricles and the His-Purkinje system and on human Na(v)1.5 in a heterologous expression system. We investigated the mechanism of channel inhibition by determining its voltage-, frequency-, state-, and temperature-dependence, complemented by a molecular drug docking to the recent Na(v)1.5 cryoEM structure. Automated patch-clamp experiments were used to investigate ivabradine-mediated changes in Na(v)1.5 inactivation parameters and inhibition of different VGSC isoforms.Key results: Ivabradine inhibited VGSCs in a voltage- and frequency-dependent manner, but did not alter voltage-dependence of activation and fast inactivation, nor recovery from fast inactivation. Cardiac (Na(v)1.5), neuronal (Na(v)1.2), and skeletal muscle (Na(v)1.4) VGSC isoforms were inhibited by ivabradine within the same concentration range, as were sodium currents in native cardiomyocytes isolated from the ventricles and the His-Purkinje system. Molecular drug docking suggested an interaction of ivabradine with the classical local anesthetic binding site.Conclusion and Implications: Ivabradine acts as an atypical inhibitor of VGSCs. Inhibition of VGSCs likely contributes to the heart rate lowering effect of ivabradine, in particular at higher stimulation frequencies and depolarized membrane potentials, and to the observed slowing of intra-cardiac conduction. Inhibition of VGSCs in native cardiomyocytes and across channel isoforms may provide a potential basis for the anti-arrhythmic potential as observed upon administration of ivabradine.",

keywords = "atypical inhibitor, conduction cell, ivabradine, S16257, ventricular cardiomyocyte, voltage-gated sodium channel, VENTRICULAR RATE, SINOATRIAL NODE, ATRIAL-FIBRILLATION, JUNCTIONAL ECTOPIC TACHYCARDIA, TARGETED DISRUPTION, FUNCTIONAL EXPRESSION, ATRIOVENTRICULAR-BLOCK, HEART-RATE REDUCTION, CARDIAC PREPARATIONS, I-F INHIBITION",

author = "Benjamin Hackl and Peter Lukacs and Janine Ebner and Krisztina Pesti and Nicholas Haechl and F{\"o}ldi, \{M{\'a}ty{\'a}s C.\} and Elena Lilliu and Klaus Schicker and Helmut Kubista and Anna Stary-Weinzinger and Karlheinz Hilber and Arpad Mike and Hannes Todt and Xaver Koenig",

note = "Publisher Copyright: Copyright {\textcopyright} 2022 Hackl, Lukacs, Ebner, Pesti, Haechl, F{\"o}ldi, Lilliu, Schicker, Kubista, Stary-Weinzinger, Hilber, Mike, Todt and Koenig.",

year = "2022",

month = may,

day = "2",

doi = "10.3389/fphar.2022.809802",

language = "English",

volume = "13",

journal = "Frontiers in Pharmacology",

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T1 - The Bradycardic Agent Ivabradine Acts as an Atypical Inhibitor of Voltage-Gated Sodium Channels

AU - Hackl, Benjamin

AU - Lukacs, Peter

AU - Ebner, Janine

AU - Pesti, Krisztina

AU - Haechl, Nicholas

AU - Földi, Mátyás C.

AU - Lilliu, Elena

AU - Schicker, Klaus

AU - Kubista, Helmut

AU - Stary-Weinzinger, Anna

AU - Hilber, Karlheinz

AU - Mike, Arpad

AU - Todt, Hannes

AU - Koenig, Xaver

PY - 2022/5/2

Y1 - 2022/5/2

N2 - Background and purpose: Ivabradine is clinically administered to lower the heart rate, proposedly by inhibiting hyperpolarization-activated cyclic nucleotide-gated cation channels in the sinoatrial node. Recent evidence suggests that voltage-gated sodium channels (VGSC) are inhibited within the same concentration range. VGSCs are expressed within the sinoatrial node and throughout the conduction system of the heart. A block of these channels thus likely contributes to the established and newly raised clinical indications of ivabradine. We, therefore, investigated the pharmacological action of ivabradine on VGSCs in sufficient detail in order to gain a better understanding of the pro- and anti-arrhythmic effects associated with the administration of this drug.Experimental Approach: Ivabradine was tested on VGSCs in native cardiomyocytes isolated from mouse ventricles and the His-Purkinje system and on human Na(v)1.5 in a heterologous expression system. We investigated the mechanism of channel inhibition by determining its voltage-, frequency-, state-, and temperature-dependence, complemented by a molecular drug docking to the recent Na(v)1.5 cryoEM structure. Automated patch-clamp experiments were used to investigate ivabradine-mediated changes in Na(v)1.5 inactivation parameters and inhibition of different VGSC isoforms.Key results: Ivabradine inhibited VGSCs in a voltage- and frequency-dependent manner, but did not alter voltage-dependence of activation and fast inactivation, nor recovery from fast inactivation. Cardiac (Na(v)1.5), neuronal (Na(v)1.2), and skeletal muscle (Na(v)1.4) VGSC isoforms were inhibited by ivabradine within the same concentration range, as were sodium currents in native cardiomyocytes isolated from the ventricles and the His-Purkinje system. Molecular drug docking suggested an interaction of ivabradine with the classical local anesthetic binding site.Conclusion and Implications: Ivabradine acts as an atypical inhibitor of VGSCs. Inhibition of VGSCs likely contributes to the heart rate lowering effect of ivabradine, in particular at higher stimulation frequencies and depolarized membrane potentials, and to the observed slowing of intra-cardiac conduction. Inhibition of VGSCs in native cardiomyocytes and across channel isoforms may provide a potential basis for the anti-arrhythmic potential as observed upon administration of ivabradine.

AB - Background and purpose: Ivabradine is clinically administered to lower the heart rate, proposedly by inhibiting hyperpolarization-activated cyclic nucleotide-gated cation channels in the sinoatrial node. Recent evidence suggests that voltage-gated sodium channels (VGSC) are inhibited within the same concentration range. VGSCs are expressed within the sinoatrial node and throughout the conduction system of the heart. A block of these channels thus likely contributes to the established and newly raised clinical indications of ivabradine. We, therefore, investigated the pharmacological action of ivabradine on VGSCs in sufficient detail in order to gain a better understanding of the pro- and anti-arrhythmic effects associated with the administration of this drug.Experimental Approach: Ivabradine was tested on VGSCs in native cardiomyocytes isolated from mouse ventricles and the His-Purkinje system and on human Na(v)1.5 in a heterologous expression system. We investigated the mechanism of channel inhibition by determining its voltage-, frequency-, state-, and temperature-dependence, complemented by a molecular drug docking to the recent Na(v)1.5 cryoEM structure. Automated patch-clamp experiments were used to investigate ivabradine-mediated changes in Na(v)1.5 inactivation parameters and inhibition of different VGSC isoforms.Key results: Ivabradine inhibited VGSCs in a voltage- and frequency-dependent manner, but did not alter voltage-dependence of activation and fast inactivation, nor recovery from fast inactivation. Cardiac (Na(v)1.5), neuronal (Na(v)1.2), and skeletal muscle (Na(v)1.4) VGSC isoforms were inhibited by ivabradine within the same concentration range, as were sodium currents in native cardiomyocytes isolated from the ventricles and the His-Purkinje system. Molecular drug docking suggested an interaction of ivabradine with the classical local anesthetic binding site.Conclusion and Implications: Ivabradine acts as an atypical inhibitor of VGSCs. Inhibition of VGSCs likely contributes to the heart rate lowering effect of ivabradine, in particular at higher stimulation frequencies and depolarized membrane potentials, and to the observed slowing of intra-cardiac conduction. Inhibition of VGSCs in native cardiomyocytes and across channel isoforms may provide a potential basis for the anti-arrhythmic potential as observed upon administration of ivabradine.

KW - atypical inhibitor

KW - conduction cell

KW - ivabradine

KW - S16257

KW - ventricular cardiomyocyte

KW - voltage-gated sodium channel

KW - VENTRICULAR RATE

KW - SINOATRIAL NODE

KW - ATRIAL-FIBRILLATION

KW - JUNCTIONAL ECTOPIC TACHYCARDIA

KW - TARGETED DISRUPTION

KW - FUNCTIONAL EXPRESSION

KW - ATRIOVENTRICULAR-BLOCK

KW - HEART-RATE REDUCTION

KW - CARDIAC PREPARATIONS

KW - I-F INHIBITION

UR - https://www.scopus.com/pages/publications/85130305926

U2 - 10.3389/fphar.2022.809802

DO - 10.3389/fphar.2022.809802

M3 - Article

SN - 1663-9812

VL - 13

JO - Frontiers in Pharmacology

JF - Frontiers in Pharmacology

M1 - 809802

ER -

The Bradycardic Agent Ivabradine Acts as an Atypical Inhibitor of Voltage-Gated Sodium Channels

Abstract

Funding

Austrian Fields of Science 2012

Keywords

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