International Journal of Molecular Sciences (Jun 2022)

miR-1183 Is a Key Marker of Remodeling upon Stretch and Tachycardia in Human Myocardium

  • Natasa Djalinac,
  • Ewald Kolesnik,
  • Heinrich Maechler,
  • Susanne Scheruebel-Posch,
  • Brigitte Pelzmann,
  • Peter P. Rainer,
  • Ines Foessl,
  • Markus Wallner,
  • Daniel Scherr,
  • Akos Heinemann,
  • Simon Sedej,
  • Senka Ljubojevic-Holzer,
  • Dirk von Lewinski,
  • Egbert Bisping

DOI
https://doi.org/10.3390/ijms23136962
Journal volume & issue
Vol. 23, no. 13
p. 6962

Abstract

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Many cardiac insults causing atrial remodeling are linked to either stretch or tachycardia, but a comparative characterization of their effects on early remodeling events in human myocardium is lacking. Here, we applied isometric stretch or sustained tachycardia at 2.5 Hz in human atrial trabeculae for 6 h followed by microarray gene expression profiling. Among largely independent expression patterns, we found a small common fraction with the microRNA miR-1183 as the highest up-regulated transcript (up to 4-fold). Both, acute stretch and tachycardia induced down-regulation of the predicted miR-1183 target genes ADAM20 and PLA2G7. Furthermore, miR-1183 was also significantly up-regulated in chronically remodeled atrial samples from patients with persistent atrial fibrillation (3-fold up-regulation versus sinus rhythm samples), and in ventricular myocardium from dilative cardiomyopathy hearts (2-fold up-regulation) as compared to non-failing controls. In sum, although stretch and tachycardia show distinct transcriptomic signatures in human atrial myocardium, both cardiac insults consistently regulate the expression of miR-1183 and its downstream targets in acute and chronic remodeling. Thus, elevated expression of miR-1183 might serve as a tissue biomarker for atrial remodeling and might be of potential functional significance in cardiac disease.

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