Generation of reentrant arrhythmias by dominant-negative inhibition of connexin43 in rat cultured myocyte monolayers

doi:10.1093/cvr/cvn084

Cardiovascular Research Advance Access originally published online on March 31, 2008
Cardiovascular Research 2008 79(1):70-79; doi:10.1093/cvr/cvn084

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Generation of reentrant arrhythmias by dominant-negative inhibition of connexin43 in rat cultured myocyte monolayers

Takuo Nakagami¹^,2, Hideo Tanaka¹^,*, Ping Dai¹, Shien-Fong Lin³, Takuji Tanabe¹, Hiroki Mani¹, Katsuji Fujiwara¹, Hiroaki Matsubara² and Tetsuro Takamatsu¹

¹ Department of Pathology and Cell Regulation, Kyoto Prefectural University of Medicine Graduate School of Medical Science, Kawaramachi Hirokoji, Kamigyo-Ku, Kyoto 602-8566, Japan
² Department of Cardiovascular Medicine, Kyoto Prefectural University of Medicine Graduate School of Medical Science, Kyoto, Japan
³ Krannert Institute of Cardiology, Indiana University School of Medicine, Indianapolis, IN, USA

^* Corresponding author. Tel: +81 75 251 5322; fax: +81 75 251 5353. E-mail address: hideotan{at}koto.kpu-m.ac.jp

Aims: Alteration of connexin43 (Cx43)-mediated intercellular communicationis known to promote susceptibility to ventricular tachyarrhythmias.However, the precise mechanism of the altered Cx43 responsiblefor arrhythmogenesis remains unclear. We sought to understandchanges in impulse propagation of ventricular myocytes underdominant-negative (DN) inhibition of Cx43 in the developmentof arrhythmias.

Methods and results: Intercellular communication was inhibited in confluent monolayersof neonatal rat cultured myocytes by an adenoviral vector-mediatedgene transfer for DNCx43-fused red fluorescence protein (RFP).A high-resolution, macro-zoom fluorescence imaging system wasused to visualize both the fluo4- and RFP-fluorescence intensitiesas measures of Ca²⁺ transient propagation and distribution ofDNCx43 inhibition, respectively, in the myocyte monolayers.DNCx43 inhibition of the monolayers resulted in not only a significantslowing of Ca²⁺ transient propagation velocity, but also a preferentialemergence of spiral-wave reentrant arrhythmias elicited by rapidpacing. Detailed observations on the development of spiral wavesrevealed that the gene-transferred myocyte monolayers exhibitedregional slowing of propagation and subsequent generation ofwave break, resulting in reentrant arrhythmias. Furthermore,DNCx43-RFP-transferred monolayers showed higher fluorescenceintensity of RFP at the break point than at the surroundingmyocardium, indicating a culprit role of DNCx43 inhibition inthe genesis of spiral reentry.

Conclusion: The present results indicate that regional heterogeneity ingap-junctional communication promotes, in addition to slowingof conduction velocity, susceptibility to reentrant tachyarrhythmias.

KEYWORDS Connexin43; Dominant-negative mutation; Myocytes; Spiral wave; Arrhythmia (mechanisms)

Time for primary review: 29 days

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