Effects of converting enzyme inhibitors on angiotensin and bradykinin peptides.

Author:

Campbell D J1,Kladis A1,Duncan A M1

Affiliation:

1. St Vincent's Institute of Medical Research, Fitzroy, Victoria, Australia.

Abstract

We examined the dose-related effects of angiotensin-converting enzyme inhibitors on circulating and tissue levels of angiotensin and bradykinin peptides by administering perindopril or lisinopril to rats in drinking water for 7 days. A reduction in the ratio of plasma angiotensin II (Ang II) to Ang I was seen for 0.006 mg/kg per day perindopril, with an increase in plasma renin and Ang I at 0.017 mg/kg per day. Plasma Ang II levels did not decrease until 1.4 mg/kg per day perindopril, at which dose plasma Ang I levels reached a plateau of an approximate 25-fold increase. The effects of perindopril on Ang II and Ang I levels in heart, lung, aorta, and brown adipose tissue were parallel to those observed for plasma. By contrast, renal Ang I levels did not increase, and renal Ang II levels decreased by 40% at 0.017 mg/kg per day, the same threshold seen for the increase in plasma renin. Perindopril increased circulating bradykinin-(1-9) levels approximately eightfold, with a threshold dose of 0.052 mg/kg per day, and increased bradykinin-(1-9) levels in kidney, heart, and lung in parallel with the changes observed for plasma. By contrast, aortic and brown adipose tissue bradykinin-(1-9) and bradykinin-(1-7) levels increased severalfold for perindopril doses as low as 0.006 mg/kg per day. Lisinopril also increased aortic bradykinin-(1-9) and bradykinin-(1-7) levels at doses below the threshold for the decrease in the ratio of Ang II to Ang I. These data indicate that renal Ang II levels and vascular bradykinin-(1-9) levels respond to low doses of converting enzyme inhibitor and may be important mediators of the effects of these compounds. The parallel increases in bradykinin-(1-9) and bradykinin-(1-7) levels in aorta and brown adipose tissue, at inhibitor doses below the threshold for inhibition of Ang I conversion, may result from a mechanism different from inhibition of "classic" angiotensin-converting enzyme.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Internal Medicine

Reference68 articles.

1. Ehlers MRW Riordan JF. Angiotensin-converting enzyme: biochemistry and molecular biology. In: Laragh JH Brenner BM eds. Hypertension: Pathophysiology Diagnosis and Management. New York NY: Raven Press Publishers; 1990:1217-1231.

2. Hansson L Dahlof B Himmelmann A Svensson A. Angiotensinconverting enzyme inhibitors in the treatment of essential hypertension. In: Robertson JIS Nicholls MG eds. The Renin-Angiotensin System. London England: Gower Medical Publishing; 1993:91.1-91.24.

3. Crozier IG Ikram H Nicholls MG. Angiotensin-converting enzyme inhibitors in the treatment of heart failure. In: Robertson JIS Nicholls MG eds. The Renin-Angiotensin System. London England: Gower Medical Publishing; 1993:93.1-93.21.

4. Crozier IG Richards AM Ikram H Nicholls MG. The reninangiotensin system ACE inhibitors and cardiac structure. In: Robertson JIS Nicholls MG eds. The Renin-Angiotensin System. London England: Gower Medical Publishing; 1993:94.1-94.10.

5. Inhibitors of Angiotensin-Converting Enzyme Prevent Myointimal Proliferation After Vascular Injury

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