Myocardial contraction is 5-fold more economical in ventricular than in atrial human tissue

doi:10.1016/j.cardiores.2004.09.029

Cardiovascular Research 2005 65(1):221-229; doi:10.1016/j.cardiores.2004.09.029

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Myocardial contraction is 5-fold more economical in ventricular than in atrial human tissue

N.A. Narolska^a^,*, R.B. van Loon^b, N.M. Boontje^a, R. Zaremba^a, S. Eiras Penas^a, J. Russell^a, S.R. Spiegelenberg^c, M.A.J.M. Huybregts^c, F.C. Visser^b, J.W. de Jong^d, J. van der Velden^a and G.J.M. Stienen^a

^aLaboratory for Physiology, Institute for Cardiovascular Research (ICaR-VU), VU University Medical Center, van der Boechorststraat 7, 1081BT Amsterdam, The Netherlands
^bDepartment of Cardiology, Institute for Cardiovascular Research (ICaR-VU), VU University Medical Center, Amsterdam, The Netherlands
^cDepartment of Cardiac Surgery, Institute for Cardiovascular Research (ICaR-VU), VU University Medical Center, Amsterdam, The Netherlands
^dThorax Center, Erasmus MC, Rotterdam, The Netherlands

^* Corresponding author. Tel.: +31 20 444 8121; fax: +31 20 444 8255. Email address: na.narolska{at}vumc.nl

Objective: Cardiac energetics and performance depend on theexpression level of the fast ( ${alpha}$ -) and slow (β-) myosin heavychain (MHC) isoform. In ventricular tissue, the β-MHC isoformpredominates, whereas in atrial tissue a variable mixture of ${alpha}$ - and β-MHC is found. In several cardiac diseases, theslow isoform is upregulated; however, the functional implicationsof this transition in human myocardium are largely unknown.The aim of this study was to determine the relation betweencontractile properties and MHC isoform composition in healthyhuman myocardium using the diversity in atrial tissue.

Methods: Isometric force production and ATP consumption weremeasured in chemically skinned atrial trabeculae and ventricularmuscle strips, and rate of force redevelopment was studied usingsingle cardiomyocytes. MHC isoform composition was determinedby one-dimensional SDS-gel electrophoresis.

Results: Force development in ventricular tissue was about 5-foldmore economical, but nine times slower, than in atrial tissue.Significant linear correlations were found between MHC isoformcomposition, ATP consumption and rate of force redevelopment.

Conclusion: These results clearly indicate that even a minorshift in MHC isoform expression has considerable impact on cardiacperformance in human tissue.

KEYWORDS Atrial function; Ventricular function; Contractile apparatus; Myocytes; Heart failure

Time for primary review 24 days

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