Hypertension, Vol 3, 59-66, Copyright © 1981 by American Heart Association
V Sreenivasan, B Walker, J Krasney, B Mookerjee and R Venuto
The renal effects of two structurally dissimilar inhibitors of
prostaglandin synthesis (Meclofenamate and RO-20-5720) were studied in
conscious, chronically instrumented dogs during mild volume expansion and
during a constant infusion of furosemide. When either inhibitor was
administered following volume expansion, urinary excretion of PGE2 and
urine flow rate were reduced by more than 50%. In contrast, renal plasma
flow fell by less than 10% while glomerular filtration rate, sodium
excretion, and plasma renin activity (PRA) were unchanged. In separate
studies, infusion of furosemide increased renal plasma flow, urine flow
rate, sodium excretion, PRA, and urinary excretion of PGE2, while
glomerular filtration rate decreased. Administration of inhibitors of
prostaglandin synthesis during constant infusion of furosemide reduced the
urinary excretion of PGE2 to control levels, as renal plasma flow and
glomerular filtration rate fell below control level. Despite these
hemodynamic alterations, the furosemide-induced diuresis and increase in
PRA were only partly attenuated by prostaglandin inhibition. It is
concluded that in conscious dogs, intrarenal prostaglandins modulate urine
flow rate during mild volume expansion and play a major role in mediating
the renal hemodynamic effects of furosemide.
ARTICLES
Role of endogenous prostaglandins in volume expansion and during furosemide infusion in conscious dogs