Contribution of angiotensin-converting enzyme to the cardiac metabolism of bradykinin: an interspecies study

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Contribution of angiotensin-converting enzyme to the cardiac metabolism of bradykinin: an interspecies study

Charles Blais Jr.¹, Guy Drapeau², Philippe Raymond¹, Daniel Lamontagne¹, Nicole Gervais¹, Ingrid Venneman, and Albert Adam¹

¹ Faculté de Pharmacie, Université de Montréal, Montreal H3C 3J7; ² Centre de Recherche (Université Laval), Hôtel-Dieu de Québec, Quebec, Quebec, Canada G1R 2J7; and Service d'Anesthésie-Réanimation, Centre Hospitalier Universitaire de Liège, B.35-B 4000, Liège, Belgium

The role of angiotensin-converting enzyme (ACE) in the metabolism of bradykinin (BK) has been studied in several tissues.However, and contrary to angiotensin I, the metabolism of BK atthe cardiac level has not been investigated. In this study, wedefine the participation of ACE in the carboxy-terminal degradationof BK in heart membranes of the dog, human, rabbit, and rat. Thecalculation of the kinetic parameters characterizing the metabolismof BK and the generated des-Arg⁹-BK can be summarized as follows: the half-life (t_1/2) of BK [dog(218 ± 32 s) > human (143 ± 9 s) = rat (150 ± 4 s) > rabbit (22± 2 s)] and of des-Arg⁹-BK [dog (1,042 ± 40 s) > human (891 ± 87 s) > rat (621 ± 65 s)> rabbit (89 ± 8 s)] both showed significant differences accordingto species. Enalaprilat, an ACE inhibitor, significantly preventedthe rapid degradation of BK and des-Arg⁹-BK in all species studied, whereas retrothiorphan, a neutralendopeptidase inhibitor, and losartan, an angiotensin II typeI receptor antagonist, did not affect this metabolism. The relativeimportance of ACE in the cardiac metabolism of BK was speciesrelated: dog (68.4 ± 3.2%) = human (72.2 ± 2.0%) > rabbit (47.7± 5.0%) = rat (45.3 ± 3.9%). ACE participation in the metabolismof des-Arg⁹-BK was as follows: rabbit (57.0 ± 4.0%) > dog (39.9 ± 8.8%) =human (25.4 ± 5.5%) = rat (36.0 ± 7.0%). The participation ofcardiac kininase I (carboxypeptidase M) in the transformationof BK into des-Arg⁹-BK was minor: human (2.6 ± 0.1%) > dog (0.9 ± 0.1%) = rabbit(1.0 ± 0.1%) = rat (1.0 ± 0.1%). These results demonstrate thatACE is the major BK-degrading enzyme in cardiac membranes. However,the metabolism of exogenous BK by heart membranes is species dependent.Our observations could explain some discrepancies regarding thecontribution of kinins in the cardioprotective effects of ACEinhibitors.

angiotensin-converting enzyme inhibitor; bradykinin metabolism; cardioprotection

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