on December 24, 2007
Published online before print December 24, 2007, doi: 10.1161/CIRCULATIONAHA.107.726752
| ||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||||
Submitted on July 9, 2007
From the Department of Cardiology, Children’s Hospital Boston (C.M.W., C.I.B.) and Department of Genetics (T.K., J.G.S., C.E.S.), Harvard Medical School, Boston, Mass; Sheba Medical Center (M.A.), Tel Aviv University, Israel; Cardiovascular Institute and Department of Medicine and Human Genetics (F.A.), University of Pittsburgh, Pittsburgh, Pa; Molecular Cardiovascular Biology (A.S., J.R.), Cincinnati Children’s Hospital Medical Center, Cincinnati, Ohio; Department of Cardiology, New York University School of Medicine (S.A.B., G.M.), New York, NY; Department of Cardiology, Friedrich-Alexander University (O.T.), Erlangen, Germany; and Howard Hughes Medical Institute (J.G.S.), Boston, Mass. * To whom correspondence should be addressed. E-mail: charles.berul{at}cardio.chboston.org.
Background—PRKAG2 mutations cause glycogen-storage cardiomyopathy, ventricular preexcitation, and conduction system degeneration. A genetic approach that utilizes a binary inducible transgenic system was used to investigate the disease mechanism and to assess preventability and reversibility of disease features in a mouse model of glycogen-storage cardiomyopathy. Methods and Results—Transgenic (Tg) mice expressing a human N488I PRKAG2 cDNA under control of the tetracycline-repressible Conclusions—Using an externally modifiable transgenic system, cardiomyopathy, cardiac dysfunction, and electrophysiological disorders were demonstrated to be reversible processes in PRKAG2 disease. Transgene suppression during early postnatal development prevented the development of accessory electrical pathways but not cardiomyopathy or conduction system degeneration. Taken together, these data provide insight into mechanisms of cardiac PRKAG2 disease and suggest that glycogen-storage cardiomyopathy can be modulated by lowering glycogen content in the heart.
Accepted on October 11, 2007
Reversibility of PRKAG2 Glycogen-Storage Cardiomyopathy and Electrophysiological Manifestations
Cordula M. Wolf MD,
-myosin heavy chain promoter underwent echocardiography, ECG, and in vivo electrophysiology studies. Transgene suppression by tetracycline administration caused a reduction in cardiac glycogen content and was initiated either prenatally (TgOFF(E-8 weeks)) or at different time points during life (TgOFF(4–16 weeks), TgOFF(8–20 weeks), and TgOFF(>20 weeks)). One group never received tetracycline, expressing transgene throughout life (TgON). TgON mice developed cardiac hypertrophy followed by dilatation, ventricular preexcitation involving multiple accessory pathways, and conduction system disease, including sinus and atrioventricular node dysfunction.
Key words: electrophysiology • cardiomyopathy • genes • glycoproteins • Wolff-Parkinson-White syndrome
Related Article:
Circulation 2008 117: 127.
This article has been cited by other articles:
 |
|
 |
|
  J.#x.;n. Farré, H. J.J. Wellens, J.#x. M. Rubio, and J. Benezet CHAPTER 28 Supraventricular Tachycardias ESC Textbook of Cardiovascular Medicine, January 1, 2009; 2(1): med-9780199566990-chapter - med-9780199566990-chapter. [Abstract] [Full Text] [PDF]
|
|
|
|
 |
|
 H. L. Tan, A. C. van der Wal, M. E. Campian, H. H. Kruyswijk, B. ten Hove Jansen, D.-J. van Doorn, H. J. Oskam, A. E. Becker, and A. A.M. Wilde Nodoventricular Accessory Pathways in PRKAG2-Dependent Familial Preexcitation Syndrome Reveal a Disorder in Cardiac Development Circ Arrhythm Electrophysiol, October 1, 2008; 1(4): 276 - 281. [Abstract] [Full Text] [PDF]
|
|
|
|
 |
|
 M. H. Gollob Modulating Phenotypic Expression of the PRKAG2 Cardiac Syndrome Circulation, January 15, 2008; 117(2): 134 - 135. [Full Text] [PDF]
|
|