Altered patterns of cardiac intercellular junction distribution in hypertrophic cardiomyopathy.

R Sepp, NJ Severs, RG Gourdie - Heart, 1996 - heart.bmj.com
R Sepp, NJ Severs, RG Gourdie
Heart, 1996heart.bmj.com
OBJECTIVE: To examine the distribution pattern of intercellular junctions (the mechanically
coupling desmosomes and the electrically coupling gap junctions) in hypertrophic
cardiomyopathy (HCM) hearts showing myofibre disarray. DESIGN: Samples from six
necropsied hearts were studied, representing the interventricular septum and the free walls
of the left and right ventricles. Immunohistochemical labelling of desmoplakin was used as a
marker for desmosomes, and of connexin43 as a marker for gap junctions, in single and …
OBJECTIVE
To examine the distribution pattern of intercellular junctions (the mechanically coupling desmosomes and the electrically coupling gap junctions) in hypertrophic cardiomyopathy (HCM) hearts showing myofibre disarray.
DESIGN
Samples from six necropsied hearts were studied, representing the interventricular septum and the free walls of the left and right ventricles. Immunohistochemical labelling of desmoplakin was used as a marker for desmosomes, and of connexin43 as a marker for gap junctions, in single and double stainings. The slides were examined by confocal laser scanning microscopy.
RESULTS
Marked disorganisation of intercalated discs was observed in areas featuring myofibre disarray. Besides overall derangement, localised abnormalities in desmosome organisation were evident, which included: (1) the formation of abnormally enlarged megadiscs; (2) the presence of intersecting disc structures; and (3) aberrant side to side desmosomal connections. Gap junctional abnormalities included: (1) random distribution of gap junctions over the surface of myocytes, rather than localisation to intercalated discs; (2) abundant side to side gap junction connections between adjacent myocytes; and (3) formation of abnormally shaped gap junctions. Circles of myocytes continuously interconnected by gap junctions were also observed. Regions of the diseased hearts lacking myofibre disarray, and control hearts of normal patients and patients with other cardiac diseases, did not show these alterations.
CONCLUSIONS
The disorganisation of the intercellular junctions associated with myofibre disarray in HCM may play an important role in the pathophysiological manifestations of the disease. The remodelling of gap junction distribution may underlie the formation of an arrhythmogenic substrate, thereby contributing to the generation and maintenance of cardiac arrhythmias associated with HCM.
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