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(Circulation. 2005;111:11-20.)
© 2005 American Heart Association, Inc.
Arrhythmia/Electrophysiology |
From the Department of Medicine, Johns Hopkins University, Baltimore, Md.
Correspondence to Ronald Li, PhD, Assistant Professor of Medicine, Johns Hopkins University, Ross 1165, 720 Rutland Ave, Baltimore MD 21205. E-mail ronaldli{at}jhmi.edu
Received August 19, 2004; revision received September 23, 2004; accepted September 30, 2004.
Background Human embryonic stem cells (hESCs) derived from blastocysts can propagate indefinitely in culture while maintaining pluripotency, including the ability to differentiate into cardiomyocytes (CMs); therefore, hESCs may provide an unlimited source of human CMs for cell-based therapies. Although CMs can be derived from hESCs ex vivo, it remains uncertain whether a functional syncytium can be formed between donor and recipient cells after engraftment.
Methods and Results Using a combination of electrophysiological and imaging techniques, here we demonstrate that electrically active, donor CMs derived from hESCs that had been stably genetically engineered by a recombinant lentivirus can functionally integrate with otherwise-quiescent, recipient, ventricular CMs to induce rhythmic electrical and contractile activities in vitro. The integrated syncytium was responsive to the ß-adrenergic agonist isoproterenol as well as to other pharmacological agents such as lidocaine and ZD7288. Similarly, a functional hESC-derived pacemaker could be implanted in the left ventricle in vivo. Detailed optical mapping of the epicardial surface of guinea pig hearts transplanted with hESC-derived CMs confirmed the successful spread of membrane depolarization from the site of injection to the surrounding myocardium.
Conclusions We conclude that electrically active, hESC-derived CMs are capable of actively pacing quiescent, recipient, ventricular CMs in vitro and ventricular myocardium in vivo. Our results may lead to an alternative or a supplemental method for correcting defects in cardiac impulse generation, such as cell-based pacemakers.
Key Words: stem cells cardiac development viruses gene therapy pacemakers
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