Affiliation:
1. From the Department of Physiology, School of Medicine, University of Florida, Gainesville.
Abstract
Background
—β-Blockers are the first line of therapy for hypertension. However, they are associated with side effects because of central nervous system (CNS) effects and β
2
-adrenergic antagonism. To overcome these problems and provide a long-term β
1
-blockade, antisense oligonucleotides against rat β
1
-adrenergic receptor (β
1
-AR) mRNA (β
1
-AS-ODN) were designed and tested for the ability to inhibit cardiac β
1
-ARs as well as lower blood pressure in spontaneously hypertensive rats (SHRs).
Methods and Results
—Radioligand binding assay showed that a single intravenous injection of β
1
-AS-ODN delivered in cationic liposomes significantly decreased cardiac β
1
-AR density by 30% to 50% for 18 days (
P
<0.01), with no effect on β
2
-ARs. This was accompanied by marked attenuation of β
1
-AR–mediated positive inotropic response in isolated perfused hearts in vitro (
P
<0.02) and in conscious SHRs monitored by telemetry in vivo (
P
<0.02). Furthermore, the blood pressure of SHRs was reduced for 20 days, with a 38 mm Hg maximum drop. Heart rate was not significantly decreased. Quantitative autoradiography was performed to assess β
1
-AS-ODN effects on the CNS, which demonstrated no changes in β
1
-ARs in brain, in contrast to a significant reduction in heart and kidney (
P
<0.05). For comparison with β-blockers, the effects of atenolol on cardiovascular hemodynamics were examined, which lowered blood pressure for only 10 hours and elicited appreciable bradycardia in SHRs.
Conclusions
—These results indicate that β
1
-AS-ODN, a novel approach to specific β
1
-blockade, has advantages over currently used β-blockers in providing a profound and prolonged reduction in blood pressure without affecting heart rate, β
2
-ARs, and the CNS. Diminished cardiac contractility resulting from less β
1
-AR expression contributes to the antihypertensive effect.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Physiology (medical),Cardiology and Cardiovascular Medicine
Cited by
46 articles.
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