Remodeling of myocyte gap junctions in arrhythmogenic right ventricular cardiomyopathy due to a deletion in plakoglobin (Naxos disease)
SR Kaplan, JJ Gard, N Protonotarios, A Tsatsopoulou… - Heart rhythm, 2004 - Elsevier
SR Kaplan, JJ Gard, N Protonotarios, A Tsatsopoulou, C Spiliopoulou, A Anastasakis…
Heart rhythm, 2004•ElsevierOBJECTIVES: We tested the hypothesis that defective interactions between adhesion
junctions and the cytoskeleton caused by the plakoglobin mutation in Naxos disease lead to
remodeling of gap junctions and altered expression of the major gap junction protein,
connexin43. BACKGROUND: Naxos disease, a recessive form of arrhythmogenic right
ventricular cardiomyopathy, is associated with a high incidence of arrhythmias and sudden
cardiac death. Naxos disease is caused by a mutation in plakoglobin, a protein that links cell …
junctions and the cytoskeleton caused by the plakoglobin mutation in Naxos disease lead to
remodeling of gap junctions and altered expression of the major gap junction protein,
connexin43. BACKGROUND: Naxos disease, a recessive form of arrhythmogenic right
ventricular cardiomyopathy, is associated with a high incidence of arrhythmias and sudden
cardiac death. Naxos disease is caused by a mutation in plakoglobin, a protein that links cell …
OBJECTIVES
We tested the hypothesis that defective interactions between adhesion junctions and the cytoskeleton caused by the plakoglobin mutation in Naxos disease lead to remodeling of gap junctions and altered expression of the major gap junction protein, connexin43.
BACKGROUND
Naxos disease, a recessive form of arrhythmogenic right ventricular cardiomyopathy, is associated with a high incidence of arrhythmias and sudden cardiac death. Naxos disease is caused by a mutation in plakoglobin, a protein that links cell-cell adhesion molecules to the cytoskeleton.
METHODS
Myocardial expression of connexin43 and other intercellular junction proteins was characterized in 4 patients with Naxos disease. Immunohistochemistry was performed in all 4 patients, and immunoblotting and electron microscopy were performed in 1 patient who died in childhood before overt arrhythmogenic right ventricular cardiomyopathy had developed.
RESULTS
Connexin43 expression at intercellular junctions was reduced significantly in both right and left ventricles in all patients with Naxos disease. Electron microscopy revealed smaller and fewer gap junctions interconnecting ventricular myocytes. Mutant plakoglobin was expressed but failed to localize normally at intercellular junctions. Localization of N-cadherin, α- and β-catenins, plakophilin-2, desmoplakin-1, and desmocollin-2 at intercalated disks appeared normal.
CONCLUSIONS
Remodeling of gap junctions occurs early in Naxos disease, presumably because of abnormal linkage between mechanical junctions and the cytoskeleton. Gap junction remodeling may produce a coupling defect which, combined with the subsequent development of pathologic changes in myocardium, could contribute to a highly arrhythmogenic substrate and enhance the risk of sudden death in Naxos disease.
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