Endothelin A-receptor antagonist administration immediately after experimental myocardial infarction with reperfusion does not affect scar healing in dogs

doi:10.1016/S0008-6363(02)00340-1

Cardiovascular Research 2002 55(1):113-121; doi:10.1016/S0008-6363(02)00340-1
© 2002 by European Society of Cardiology

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Endothelin A-receptor antagonist administration immediately after experimental myocardial infarction with reperfusion does not affect scar healing in dogs

Cristina Basso^a, Gaetano Thiene^a^,*, Mila Della Barbera^a, Annalisa Angelini^a, Michael Kirchengast^b^,c and Sabino Iliceto^d

^aInstitute of Pathological Anatomy, University of Padua Medical School, Via A. Gabelli 61, 35121 Padova, Italy
^bInstitute of Pharmacology and Toxicology, University of Heidelberg Medical School, Mannheim, Germany
^cCardion AG, Erkrath, Germany
^dDivision of Cardiology, University of Padua Medical School, Padova, Italy

cardpath{at}unipd.it

^* Corresponding author. Tel.: +39-049-827-2283; fax: +39-049-827-2284

Objective: Endothelin (ET) receptor antagonists have been reportedto reduce both infarct size and no-reflow phenomenon; however,in rat models their effect on the healing process after myocardialinfarction (MI) is controversial. The study aimed to evaluatethe effect of early administration of the ET_A receptor antagonistdarusentan on scar healing in an ischemia-reperfusion modelin dogs. Methods: Thirty male mongrel dogs surviving 180 minleft anterior descending coronary artery balloon occlusion wererandomised to: darusentan i.v. bolus—5 mg/kg 5 min beforereperfusion—(group I); darusentan i.v. bolus+chronic oral—10mg/kg/day—(group II); saline (group III). Five age-matcheddogs served as controls (group IV). At 6 weeks weight, volume,mass/volume, wall thickness, thinning ratio and expansion indexwere assessed in the explanted hearts. Infarct size and scararea tissue composition were evaluated by computerized histomorphometry.Cellularity, vessels and TGFβ in the scar area were scoredby immunohistochemistry. Results: 24 dogs (80%; 7 group I, 8group II, 9 group III) developed an anterior MI, transmuralin 15 and subendocardial in 9, mean size 11.5±4% of leftventricular area and 37±9% of left ventricular endocardialcircumference. MIs were homogeneously distributed among thethree groups regarding either infarct size or transmural extent.No differences were found in the three MI groups regarding thinningratio, expansion index and scar area tissue characterization.Percent scar collagen content (37±17 vs. 53±20vs. 46±14), myofibroblasts (1.2 vs. 1.3 vs. 1.4), macrophages(1.2±0.5 vs. 1.3±0.5 vs. 1.4±0.5), neovessels(2.8±0.4 vs. 2.6±0.5 vs. 2.9±0.3) and TGFβscore (2 vs. 2.25 vs. 2.11) were not significantly different.Conclusions: Early administration of the ET_A receptor antagonistdarusentan does not affect the scar healing process at 6 weeksafter experimental MI with reperfusion in dogs.

KEYWORDS Endothelins; Fibrosis; Histo(patho)logy; Infarction; Reperfusion

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