Hypertension, Vol 9, 467-472, Copyright © 1987 by American Heart Association
WR Davidson Jr, S Kawashima, SP Banerjee and CS Liang
To determine the mechanism of blunted sympathetic reflex responses in early
renovascular hypertension, we measured inotropic and chronotropic responses
of the heart to beta-adrenergic stimulation in vivo and myocardial
beta-adrenergic receptor number and adenylate cyclase activity in 10 dogs
during an early stage of one-kidney renal hypertension. Mean aortic
pressure was higher in the hypertensive dogs (152 +/- 4 mm Hg) than in
eight sham-operated dogs (122 +/- 1 mm Hg; p less than 0.001), but heart
rate, cardiac output, and left atrial pressure did not differ between the
two groups. Blood pressure reduction with a direct-acting vasodilator,
pinacidil, resulted in marked increases in heart rate (+97 +/- 12
beats/min) and rate of change of left ventricular pressure (dP/dt; +1447
+/- 367 mm Hg/sec) in normotensive dogs but only blunted heart rate (+54
+/- 12 beats/min) and minimal left ventricular dP/dt (+376 +/- 264 mm
Hg/sec) responses in hypertensive dogs. In contrast, intravenously
administered isoproterenol produced similar increases in heart rate and
left ventricular dP/dt in the two groups. These two groups also did not
differ in either left ventricular beta-adrenergic receptor number and
affinity or basal, isoproterenol-stimulated, and fluoride-stimulated
adenylate cyclase activity. Thus, despite blunted reflex responses to blood
pressure reduction, hypertensive dogs showed neither reduction in
chronotropic and inotropic responses to direct beta-adrenergic stimulation
nor beta-adrenergic desensitization of the myocardium, as assessed by
beta-adrenergic receptor number and adenylate cyclase activity. Blunted
reflex responses in this model of early hypertension must be due to factors
operating at some locus other than the beta- adrenergic receptor-adenylate
cyclase complex.
ARTICLES
Preserved cardiac beta-adrenergic sensitivity in early renovascular hypertension