Tissue engineering of functional cardiac muscle: molecular, structural, and electrophysiological studies

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Tissue engineering of functional cardiac muscle: molecular, structural, and electrophysiological studies

M. Papadaki¹^,^*, N. Bursac¹^,⁴^,^*, R. Langer¹^,², J. Merok³, G. Vunjak-Novakovic¹, and L. E. Freed¹

¹ Division of Health Sciences and Technology and Departments of ² Chemical Engineering and ³ Biology, Massachusetts Institute of Technology, Cambridge 02139; and ⁴ Department of Biomedical Engineering, Boston University, Boston, Massachusetts 02215

The primary aim of this study was to relate molecular and structural properties of in vitro reconstructed cardiac musclewith its electrophysiological function using an in vitro modelsystem based on neonatal rat cardiac myocytes, three-dimensionalpolymeric scaffolds, and bioreactors. After 1 wk of cultivation,we found that engineered cardiac muscle contained a 120- to 160-µm-thickperipheral region with cardiac myocytes that were electricallyconnected through gap junctions and sustained macroscopicallycontinuous impulse propagation over a distance of 5 mm. Molecular,structural, and electrophysiological properties were found tobe interrelated and depended on specific model system parameterssuch as the tissue culture substrate, bioreactor, and culturemedium. Native tissue and the best experimental group (engineeredcardiac muscle cultivated using laminin-coated scaffolds, rotatingbioreactors, and low-serum medium) were comparable with respectto the conduction velocity of propagated electrical impulses andspatial distribution of connexin43. Furthermore, the structuraland electrophysiological properties of the engineered cardiacmuscle, such as cellularity, conduction velocity, maximum signalamplitude, capture rate, and excitation threshold, were significantlyimproved compared with our previousstudies.

myocyte; bioreactor; laminin; serum; electrophysiology; creatine kinase-MM; myosin heavy chain; connexin43

^* Authors contributed equally to thiswork.

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