Pilot studies in our laboratory revealed that furosemide-induced renin-angiotensin-aldosterone system (RAAS) activation was not attenuated by the subsequent co-administration of benazepril. This study was designed to evaluate the effect of benazepril on angiotensin-converting enzyme (ACE) activity and furosemide-induced circulating RAAS activation. Our hypothesis was that benazepril suppression of ACE activity would not suppress furosemide-induced circulating RAAS activation, indicated by urinary aldosterone concentration. Ten healthy hound dogs were used in this study. The effect of furosemide (2mg/kg p.o., q12h; Group F; n=5) and furosemide plus benazepril (1mg/kg p.o., q24h; Group FB; n=5) on circulating RAAS was determined by plasma ACE activity, 4-6h posttreatment, and urinary aldosterone to creatinine ratio (UAldo:C) on days -1, -2, 1, 3, and 7. There was a significant increase in the average UAldo:C (g/g) after the administration of furosemide (Group F baseline [average of days -1 and -2] UAldo:C=0.41, SD 0.15; day 1 UAldo:C=1.1, SD 0.56; day 3 UAldo:C=0.85, SD 0.50; day 7 UAldo:C=1.1, SD 0.80, P<0.05). Benazepril suppressed ACE activity (U/L) in Group FB (Group FB baseline ACE=16.4, SD 4.2; day 1 ACE=3.5, SD 1.4; day 3 ACE=1.6, SD 1.3; day 7 ACE=1.4, SD 1.4, P<0.05) but did not significantly reduce aldosterone excretion (Group FB baseline UAldo:C=0.35, SD 0.16; day 1 UAldo:C=0.79, SD 0.39; day 3 UAldo:C 0.92, SD 0.48, day 7 UAldo:C=0.99, SD 0.48, P<0.05). Benazepril decreased plasma ACE activity but did not prevent furosemide-induced RAAS activation, indicating aldosterone breakthrough (escape). This is particularly noteworthy in that breakthrough is observed at the time of initiation of RAAS suppression, as opposed to developing after months of therapy.

• 出版日期2015-2