Scientific Reports (May 2018)

Overexpression of Cx43 in cells of the myocardial scar: Correction of post-infarct arrhythmias through heterotypic cell-cell coupling

  • Wilhelm Roell,
  • Alexandra M. Klein,
  • Martin Breitbach,
  • Torsten S. Becker,
  • Ashish Parikh,
  • Jane Lee,
  • Katrin Zimmermann,
  • Shaun Reining,
  • Beth Gabris,
  • Annika Ottersbach,
  • Robert Doran,
  • Britta Engelbrecht,
  • Miriam Schiffer,
  • Kenichi Kimura,
  • Patricia Freitag,
  • Esther Carls,
  • Caroline Geisen,
  • Georg D. Duerr,
  • Philipp Sasse,
  • Armin Welz,
  • Alexander Pfeifer,
  • Guy Salama,
  • Michael Kotlikoff,
  • Bernd K. Fleischmann

DOI
https://doi.org/10.1038/s41598-018-25147-8
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 14

Abstract

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Abstract Ventricular tachycardia (VT) is the most common and potentially lethal complication following myocardial infarction (MI). Biological correction of the conduction inhomogeneity that underlies re-entry could be a major advance in infarction therapy. As minimal increases in conduction of infarcted tissue markedly influence VT susceptibility, we reasoned that enhanced propagation of the electrical signal between non-excitable cells within a resolving infarct might comprise a simple means to decrease post-infarction arrhythmia risk. We therefore tested lentivirus-mediated delivery of the gap-junction protein Connexin 43 (Cx43) into acute myocardial lesions. Cx43 was expressed in (myo)fibroblasts and CD45+ cells within the scar and provided prominent and long lasting arrhythmia protection in vivo. Optical mapping of Cx43 injected hearts revealed enhanced conduction velocity within the scar, indicating Cx43-mediated electrical coupling between myocytes and (myo)fibroblasts. Thus, Cx43 gene therapy, by direct in vivo transduction of non-cardiomyocytes, comprises a simple and clinically applicable biological therapy that markedly reduces post-infarction VT.