Premium
Peripheral α 2 ‐adrenoceptor‐mediated sympathoinhibitory effects of mivazerol
Author(s) -
Richer C.,
Gobert J.,
Noyer M.,
Wülfert E.,
Giudicelli JF
Publication year - 1996
Publication title -
fundamental and clinical pharmacology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.655
H-Index - 73
eISSN - 1472-8206
pISSN - 0767-3981
DOI - 10.1111/j.1472-8206.1996.tb00611.x
Subject(s) - medicine , postsynaptic potential , hemodynamics , stimulation , agonist , sympathetic nervous system , yohimbine , endocrinology , peripheral , blood pressure , heart rate , neurotransmitter , clonidine , anesthesia , receptor , antagonist
Summary— Mivazerol is a new compound that could potentially reduce perioperative cardiovascular morbidity and mortality in patients with or at risk of coronary disease and submitted to surgery. This action of mivazerol depends on a well documented centrally mediated reduction in sympathetic nerve activity, but a direct peripheral decrease in sympathetic neurotransmitter release induced by activation of prejunctional α 2 ‐adrenoceptors located on sympathetic nerve endings could also contribute. To investigate this issue, the effects of mivazerol on the pressor, systemic and regional hemodynamic (pulsed Doppler technique) as well as on the cardiac responses to electrical stimulation of the spinal cord (SCS) were measured in pithed rats in the absence and in the presence of mivazerol. Mivazerol exerted strong sympathoinhibitory effects: SCS‐induced increases in blood pressure, total peripheral resistance and heart rate were dose‐dependently reduced by mivazerol, but among the regional vascular beds investigated, only the hindlimb vasoconstrictor responses were significantly drug‐affected. All these sympathoinhibitory effects of mivazerol were abolished by prior yohimbine administration. Simultaneously, mivazerol did not induce any postjunctional adrenoceptor blockade as it did not affect noradrenaline cardiac and hemodynamic effects. On the contrary, through postjunctional α 2 ‐adrenoceptor stimulation, mivazerol, in this pithed preparation, dose‐dependently increased blood pressure, total peripheral and hindlimb vascular resistances, but heart rate was not affected. We conclude that, in the pithed rat, mivazerol exerts strong peripheral sympathoinhibitory effects. The mechanism involved is prejunctional α 2 ‐adrenoceptor activation as i) mivazerol does not display any postsynaptic α‐adrenoceptor blocking effect — it even behaves as a postsynaptic α 2 ‐adrenoceptor agonist — and ii) yohimbine abolishes mivazerol's sympathoinhibitory effects. Thus, direct peripheral together with central mechanisms contribute to mivazerol's sympathoinhibitory effects and ultimately to its cardioprotective action.