Changes in vascular reactivity following administration of isoproterenol for 1 week: a role for endothelial modulation

Changes in vascular reactivity following administration of isoproterenol for 1 week: a role for endothelial modulation

1 The aim of this study was to assess the effects of treatment with isoproterenol (ISO, 0.3 mg kg−1 day−1, s.c.) for 7 days on the vascular reactivity of rat‐isolated aortic rings. Additionally, potential mechanisms underlying the changes that involved the endothelial modulation of contractility wer...

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Bibliographic Details
Published in:British journal of pharmacology Vol. 148; no. 5; pp. 629 - 639
Main Authors: Davel, Ana Paula C, Kawamoto, Elisa Mitiko, Scavone, Cristoforo, Vassallo, Dalton V, Rossoni, Luciana V
Format: Journal Article
Language:English
Published: Oxford, UK Blackwell Publishing Ltd 01-07-2006
Nature Publishing
Nature Publishing Group
Subjects:
Animals
Antioxidants - metabolism
Aorta, Thoracic - drug effects
Biological and medical sciences
Blood Pressure - drug effects
Blood Vessels - drug effects
endothelium
Endothelium, Vascular - drug effects
Endothelium, Vascular - physiology
Heart Rate - drug effects
Heart Ventricles - drug effects
In Vitro Techniques
Isoproterenol
Isoproterenol - administration & dosage
Male
Medical sciences
nitric oxide
Nitric Oxide Synthase - metabolism
Organ Size - drug effects
Pharmacology. Drug treatments
Phenylephrine - pharmacology
Rats
Rats, Wistar
Signal Transduction
superoxide anions
Superoxides - metabolism
vascular reactivity
Vasoconstriction - drug effects
Vasoconstrictor Agents - metabolism
β‐adrenoceptor
Agonist
Isoprenaline
Bronchodilator
β-adrenoceptor
vascular reactivity
β2-Adrenergic receptor
β-Adrenergic receptor agonist
Isoproterenol
Endothelium
β-Adrenergic receptor
Anions
Hyperoxides
Nitric oxide
superoxide anions
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Summary:1 The aim of this study was to assess the effects of treatment with isoproterenol (ISO, 0.3 mg kg−1 day−1, s.c.) for 7 days on the vascular reactivity of rat‐isolated aortic rings. Additionally, potential mechanisms underlying the changes that involved the endothelial modulation of contractility were investigated. 2 Treatment with ISO induced cardiac hypertrophy without changes in haemodynamic parameters. Aortic rings from ISO‐treated rats showed an increase in the contraction response to phenylephrine (PHE) and serotonin, but did not change relaxations produced by acetylcholine or isoproterenol. Removal of the endothelium increased the responses to PHE in both groups. However, this procedure was less effective in ISO‐treated as compared with control rats. Endothelial cell removal abolished the increase in the response to PHE in ISO‐treated rats. The presence of Nω‐nitro‐L‐arginine methyl ester shifted the concentration–response curve to PHE to the left in both groups of rats. However, this effect was more pronounced in the ISO group. In addition, aminoguanidine (50 μM) potentiated the actions of PHE only in the ISO group. ISO treatment increased nitric oxide synthase (NOS) activity and neuronal NOS and endothelial NOS protein expression in the aorta. 3 Neither losartan (10 μM) nor indomethacin (10 μM) abolished the effects of ISO on the actions of PHE. Superoxide dismutase (SOD, 150 U ml−1) and L‐arginine (5 mM), but neither catalase (300 U ml−1) nor apocynin (100 μM), blocked the effect of ISO treatment. In addition, we observed an increase in superoxide anion levels as measured by ethidium bromide fluorescence and of copper and zinc superoxide dismutase protein expression in ISO‐treated rats. 4 In conclusion, our data suggest that ISO treatment alters the endothelial cell‐mediated modulation of the contraction to PHE in rat aorta. The increased maximal response of PHE seems to be due to an increase in superoxide anion generation, which inactivates some of the basal NO produced and counteracts NO‐mediated negative modulation even in the presence of high NO production and antioxidant defence. British Journal of Pharmacology (2006) 148, 629–639. doi:10.1038/sj.bjp.0706749
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ISSN:0007-1188
1476-5381
DOI:10.1038/sj.bjp.0706749