Hypertension, Vol 7, 963-971, Copyright © 1985 by American Heart Association
A Gerber, P Weidmann, C Marone, D Uehlinger and W Riesen
Increased sympathetic activity or vascular reactivity to norepinephrine or
both may play a complementary role in the pathogenesis of essential
hypertension. Therefore, blood pressure regulation and metabolic correlates
of cardiovascular risk were evaluated in 19 normal subjects and in 13
subjects with essential hypertension receiving placebo and after 4 weeks of
intervention with urapidil, an agent that was found experimentally to exert
a combined central sympathetic and peripheral alpha-adrenergic receptor
inhibition. In hypertensive patients, urapidil normalized the initially low
norepinephrine pressor dose (+ 106%), mildly increased basal plasma
norepinephrine levels (+36%), and markedly shifted the plasma
norepinephrine concentration-blood pressure response curve (p less than
0.01). Blood pressure was decreased (p less than 0.001). In normal
subjects, urapidil produced only mild increases in norepinephrine plasma
levels (+22%) and norepinephrine pressor dose (+38%) and no change in blood
pressure. Body weight, exchangeable sodium, and blood volume were unaltered
or increased slightly. Heart rate; plasma epinephrine, renin, angiotensin
II, basal aldosterone, and electrolyte levels; plasma clearances of
norepinephrine and angiotensin II; pressor effects of angiotensin II;
chronotropic responses to isoproterenol or a norepinephrine-induced rise in
blood pressure; and urinary prostaglandin F2 alpha excretion, as well as
serum lipoprotein fractions and glucose, insulin, and uric acid levels,
were not significantly modified by urapidil. Prostaglandin E2 excretion
tended to be increased. Aldosterone responsiveness to angiotensin II was
increased by urapidil in normal (p less than 0.05) but not in hypertensive
subjects.(ABSTRACT TRUNCATED AT 250 WORDS)
ARTICLES
Cardiovascular and metabolic profile during intervention with urapidil in humans