Literature DB >> 27510622

Potassium channels in the Cx43 gap junction perinexus modulate ephaptic coupling: an experimental and modeling study.

Rengasayee Veeraraghavan1, Joyce Lin2, James P Keener3, Robert Gourdie4,5, Steven Poelzing6,7.   

Abstract

It was recently demonstrated that cardiac sodium channels (Nav1.5) localized at the perinexus, an intercalated disc (ID) nanodomain associated with gap junctions (GJ), may contribute to electrical coupling between cardiac myocytes via an ephaptic mechanism. Impairment of ephaptic coupling by acute interstitial edema (AIE)-induced swelling of the perinexus was associated with arrhythmogenic, anisotropic conduction slowing. Given that Kir2.1 has also recently been reported to localize at intercalated discs, we hypothesized that Kir2.1 channels may reside within the perinexus and that inhibiting them may mitigate arrhythmogenic conduction slowing observed during AIE. Using gated stimulated emission depletion (gSTED) and stochastic optical reconstruction microscopy (STORM) super-resolution microscopy, we indeed find that a significant proportion of Kir2.1 channels resides within the perinexus. Moreover, whereas Nav1.5 inhibition during AIE exacerbated arrhythmogenic conduction slowing, inhibiting Kir2.1 channels during AIE preferentially increased transverse conduction velocity-decreasing anisotropy and ameliorating arrhythmia risk compared to AIE alone. Comparison of our results with a nanodomain computer model identified enrichment of both Nav1.5 and Kir2.1 at intercalated discs as key factors underlying the experimental observations. We demonstrate that Kir2.1 channels are localized within the perinexus alongside Nav1.5 channels. Further, targeting Kir2.1 modulates intercellular coupling between cardiac myocytes, anisotropy of conduction, and arrhythmia propensity in a manner consistent with a role for ephaptic coupling in cardiac conduction. For over half a century, electrical excitation in the heart has been thought to occur exclusively via gap junction-mediated ionic current flow between cells. Further, excitation was thought to depend almost exclusively on sodium channels with potassium channels being involved mainly in returning the cell to rest. Here, we demonstrate that sodium and potassium channels co-reside within nanoscale domains at cell-to-cell contact sites. Experimental and computer modeling results suggest a role for these channels in electrical coupling between cardiac muscle cells via an ephaptic mechanism working in tandem with gap junctions. This new insight into the mechanism of cardiac electrical excitation could pave the way for novel therapies against cardiac rhythm disturbances.

Entities:  

Keywords:  Arrhythmia; Cardiac conduction; Ephaptic coupling; Gap junctions; Potassium channels; Sodium channels

Mesh:

Substances:

Year:  2016        PMID: 27510622      PMCID: PMC5131566          DOI: 10.1007/s00424-016-1861-2

Source DB:  PubMed          Journal:  Pflugers Arch        ISSN: 0031-6768            Impact factor:   3.657


  32 in total

1.  Localization of sodium channels in intercalated disks modulates cardiac conduction.

Authors:  Jan P Kucera; Stephan Rohr; Yoram Rudy
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2.  Distribution and three-dimensional structure of intercellular junctions in canine myocardium.

Authors:  R H Hoyt; M L Cohen; J E Saffitz
Journal:  Circ Res       Date:  1989-03       Impact factor: 17.367

3.  Ephaptic conduction in a cardiac strand model with 3D electrodiffusion.

Authors:  Yoichiro Mori; Glenn I Fishman; Charles S Peskin
Journal:  Proc Natl Acad Sci U S A       Date:  2008-04-23       Impact factor: 11.205

4.  Ephaptic coupling in cardiac myocytes.

Authors:  Joyce Lin; James P Keener
Journal:  IEEE Trans Biomed Eng       Date:  2013-02       Impact factor: 4.538

5.  Cx43 associates with Na(v)1.5 in the cardiomyocyte perinexus.

Authors:  J Matthew Rhett; Emily L Ongstad; Jane Jourdan; Robert G Gourdie
Journal:  J Membr Biol       Date:  2012-07-19       Impact factor: 1.843

6.  Ultrastructure of the intercellular space in adult murine ventricle revealed by quantitative tomographic electron microscopy.

Authors:  Alejandra Leo-Macías; Feng-Xia Liang; Mario Delmar
Journal:  Cardiovasc Res       Date:  2015-06-25       Impact factor: 10.787

7.  K+ channel blocking actions of flecainide compared with those of propafenone and quinidine in adult rat ventricular myocytes.

Authors:  M T Slawsky; N A Castle
Journal:  J Pharmacol Exp Ther       Date:  1994-04       Impact factor: 4.030

8.  Combined reduction of intercellular coupling and membrane excitability differentially affects transverse and longitudinal cardiac conduction.

Authors:  Mèra Stein; Toon A B van Veen; Carol Ann Remme; Mohamed Boulaksil; Maartje Noorman; Leonie van Stuijvenberg; Roel van der Nagel; Connie R Bezzina; Richard N W Hauer; Jacques M T de Bakker; Harold V M van Rijen
Journal:  Cardiovasc Res       Date:  2009-04-22       Impact factor: 10.787

Review 9.  Basic mechanisms of cardiac impulse propagation and associated arrhythmias.

Authors:  André G Kléber; Yoram Rudy
Journal:  Physiol Rev       Date:  2004-04       Impact factor: 37.312

10.  Sodium channels in the Cx43 gap junction perinexus may constitute a cardiac ephapse: an experimental and modeling study.

Authors:  Rengasayee Veeraraghavan; Joyce Lin; Gregory S Hoeker; James P Keener; Robert G Gourdie; Steven Poelzing
Journal:  Pflugers Arch       Date:  2015-01-13       Impact factor: 3.657

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  22 in total

1.  Intramolecular signaling in a cardiac connexin: Role of cytoplasmic domain dimerization.

Authors:  Andrew J Trease; Juan M V Capuccino; Jorge Contreras; Andrew L Harris; Paul L Sorgen
Journal:  J Mol Cell Cardiol       Date:  2017-07-25       Impact factor: 5.000

2.  Attenuating loss of cardiac conduction during no-flow ischemia through changes in perfusate sodium and calcium.

Authors:  Gregory S Hoeker; Carissa C James; Allison N Tegge; Robert G Gourdie; James W Smyth; Steven Poelzing
Journal:  Am J Physiol Heart Circ Physiol       Date:  2020-07-17       Impact factor: 4.733

3.  Distribution of cardiac sodium channels in clusters potentiates ephaptic interactions in the intercalated disc.

Authors:  Echrak Hichri; Hugues Abriel; Jan P Kucera
Journal:  J Physiol       Date:  2018-01-09       Impact factor: 5.182

4.  Intercellular Sodium Regulates Repolarization in Cardiac Tissue with Sodium Channel Gain of Function.

Authors:  Madison B Nowak; Amara Greer-Short; Xiaoping Wan; Xiaobo Wu; Isabelle Deschênes; Seth H Weinberg; Steven Poelzing
Journal:  Biophys J       Date:  2020-04-21       Impact factor: 4.033

5.  Automaticity in ventricular myocyte cell pairs with ephaptic and gap junction coupling.

Authors:  Cheng Ly; Seth H Weinberg
Journal:  Chaos       Date:  2022-03       Impact factor: 3.642

6.  Initiation and entrainment of multicellular automaticity via diffusion limited extracellular domains.

Authors:  Steven Poelzing; Seth H Weinberg; James P Keener
Journal:  Biophys J       Date:  2021-10-30       Impact factor: 4.033

7.  Tmem65 is critical for the structure and function of the intercalated discs in mouse hearts.

Authors:  Liyang Gu; Michelle Di Paola; Robert Lakin; Allen C T Teng; Zachary J Williams; Aaron Au; Wenliang Chen; Neal I Callaghan; Farigol Hakem Zadeh; Yu-Qing Zhou; Meena Fatah; Diptendu Chatterjee; L Jane Jourdan; Jack Liu; Craig A Simmons; Thomas Kislinger; Christopher M Yip; Peter H Backx; Robert G Gourdie; Robert M Hamilton; Anthony O Gramolini
Journal:  Nat Commun       Date:  2022-10-18       Impact factor: 17.694

Review 8.  Subcellular trafficking and endocytic recycling of KATP channels.

Authors:  Hua-Qian Yang; Fabio A Echeverry; Assmaa ElSheikh; Ivan Gando; Sophia Anez Arredondo; Natalie Samper; Timothy Cardozo; Mario Delmar; Show-Ling Shyng; William A Coetzee
Journal:  Am J Physiol Cell Physiol       Date:  2022-05-04       Impact factor: 5.282

9.  Intercalated disk nanoscale structure regulates cardiac conduction.

Authors:  Nicolae Moise; Heather L Struckman; Celine Dagher; Rengasayee Veeraraghavan; Seth H Weinberg
Journal:  J Gen Physiol       Date:  2021-07-15       Impact factor: 4.086

10.  Reciprocal Modulation of IK1-INa Extends Excitability in Cardiac Ventricular Cells.

Authors:  Anthony Varghese
Journal:  Front Physiol       Date:  2016-11-15       Impact factor: 4.566

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