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Comparison of zofenopril and lisinopril to study the role of the sulfhydryl‐group in improvement of endothelial dysfunction with ACE‐inhibitors in experimental heart failure
Author(s) -
Buikema H,
Monnink S H J,
Tio R A,
Crijns H J G M,
De Zeeuw D,
Van Gilst W H
Publication year - 2000
Publication title -
british journal of pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.432
H-Index - 211
eISSN - 1476-5381
pISSN - 0007-1188
DOI - 10.1038/sj.bjp.0703498
Subject(s) - lisinopril , heart failure , endothelial dysfunction , medicine , stimulation , chemistry , endocrinology , vasoprotective , vasodilation , pharmacology , endothelium , ace inhibitor , angiotensin converting enzyme , nitric oxide , blood pressure
We evaluated the role of SH‐groups in improvement of endothelial dysfunction with ACE‐inhibitors in experimental heart failure. To this end, we compared the vasoprotective effect of chronic treatment with zofenopril (plus SH‐group) versus lisinopril (no SH‐group), or N‐acetylcysteine (only SH‐group) in myocardial infarcted (MI) heart failure rats. After 11 weeks of treatment, aortas were obtained and studied as ring preparations for endothelium‐dependent and ‐independent dilatation in continuous presence of indomethacin to avoid interference of vasoactive prostanoids, and the selective presence of the NOS‐inhibitor L‐NMMA to determine NO‐contribution. Total dilatation after receptor‐dependent stimulation with acetylcholine (ACh) was attenuated (−49%, P <0.05) in untreated MI ( n =11), compared to control rats with no‐MI ( n =8). This was in part due to impaired NO‐contribution in MI (−50%, P <0.05 versus no‐MI). At the same time the capacity for generation of biologically active NO after receptor‐independent stimulation with A23187 remained intact. Chronic treatment with n‐acetylcysteine ( n =8) selectively restored NO‐contribution in total dilatation to ACh. In contrast, both ACE‐inhibitors fully normalized total dilatation to ACh, including the part mediated by NO (no significant differences between zofenopril ( n =10) and lisinopril ( n =8)). Zofenopril, but not lisinopril, additionally potentiated the effect of endogenous NO after A23187‐induced release from the endothelium (+100%) as well as that of exogenous NO provided by nitroglycerin (+22%) and sodium nitrite (+36%) (for all P <0.05 versus no‐MI). We conclude that ACE‐inhibition with a SH‐group has a potential advantage in improvement of endothelial dysfunction through increased activity of NO after release from the endothelium into the vessel wall. Furthermore, this is the first study demonstrating the selective normalizing effect of N‐actylcysteine on NO‐contribution to ACh‐induced dilatation in experimental heart failure.British Journal of Pharmacology (2000) 130 , 1999–2007; doi: 10.1038/sj.bjp.0703498