TY - JOUR
T1 - Inhibition of basic leucine zipper transcription is a major mediator of atrial dilatation
AU - Kehat, Izhak
AU - Heinrich, Ronit
AU - Ben-Izhak, Ofer
AU - Miyazaki, Hiroshi
AU - Gutkind, J. Silvio
AU - Aronheim, Ami
N1 - Funding Information:
The authors wish to thank Ms. A. Cohen and Mr. R. Lavi for their excellent technical assistance, Drs. O. Shenker and I. Suss-Toby for imaging support, and Profs. T. Hai, Chen, J., E. Beyer, E. Keshet, H. Bujard for various plasmids and reagents. This work was supported by a UICC American Cancer Society International Fellowship for Beginning Investigators and by the Israel Cancer Research Foundation and The Israel Ministry of Health grant to AA.
PY - 2006/6/1
Y1 - 2006/6/1
N2 - Objective: Atrial fibrillation is the most prevalent clinically significant cardiac arrhythmia. Atrial dilatation, a predictor of atrial fibrillation, is thought to result from increased ventricular pressure. However, the underlying molecular mechanisms responsible for atrial dilatation are largely unknown. Here we sought to examine whether the expression of a basic leucine zipper inhibitor protein, JDP2, in the heart is sufficient for the generation of atrial dilatation. Methods: A tetracycline-regulated transgene was used to express JDP2 specifically in the mouse heart. Mice hearts were dissected and subjected to Northern and Western analysis, or analyzed by ECG recording and echocardiography. Regulation of gene expression was studied using electromobility shift assays and luciferase gene reporter analysis. Results: Expression of JDP2 resulted in massive bi-atrial dilatation, defects in conduction, and a lethal phenotype. These effects were developmentally independent, acquired during adulthood, and were reversible upon abolishing of JDP2 expression. Connexin 40 and myosin light chain 2a expression were identified as potential target genes. Conclusion: Expression of basic leucine zipper transcription inhibitors is sufficient to results in atrial dilatation. This dilatation is acquired postnatally and is reversible. Thus, basic leucine zipper transcription inhibitors may be a relevant therapeutic target for preventing atrial dilatation and atrial fibrillation.
AB - Objective: Atrial fibrillation is the most prevalent clinically significant cardiac arrhythmia. Atrial dilatation, a predictor of atrial fibrillation, is thought to result from increased ventricular pressure. However, the underlying molecular mechanisms responsible for atrial dilatation are largely unknown. Here we sought to examine whether the expression of a basic leucine zipper inhibitor protein, JDP2, in the heart is sufficient for the generation of atrial dilatation. Methods: A tetracycline-regulated transgene was used to express JDP2 specifically in the mouse heart. Mice hearts were dissected and subjected to Northern and Western analysis, or analyzed by ECG recording and echocardiography. Regulation of gene expression was studied using electromobility shift assays and luciferase gene reporter analysis. Results: Expression of JDP2 resulted in massive bi-atrial dilatation, defects in conduction, and a lethal phenotype. These effects were developmentally independent, acquired during adulthood, and were reversible upon abolishing of JDP2 expression. Connexin 40 and myosin light chain 2a expression were identified as potential target genes. Conclusion: Expression of basic leucine zipper transcription inhibitors is sufficient to results in atrial dilatation. This dilatation is acquired postnatally and is reversible. Thus, basic leucine zipper transcription inhibitors may be a relevant therapeutic target for preventing atrial dilatation and atrial fibrillation.
KW - Connexins
KW - Gene expression
KW - Hypertrophy
KW - Trial function
UR - http://www.scopus.com/inward/record.url?scp=33646533285&partnerID=8YFLogxK
U2 - 10.1016/j.cardiores.2006.02.018
DO - 10.1016/j.cardiores.2006.02.018
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AN - SCOPUS:33646533285
SN - 0008-6363
VL - 70
SP - 543
EP - 554
JO - Cardiovascular Research
JF - Cardiovascular Research
IS - 3
ER -