血管紧张素转换酶在内肽酶24.15抑制剂血管效应中的作用。

Role of angiotensin converting enzyme in the vascular effects of an endopeptidase 24.15 inhibitor.

作者信息

Telford S E, Smith A I, Lew R A, Perich R B, Madden A C, Evans R G

机构信息

Baker Medical Research Institute, Prahran, Victoria, Australia.

出版信息

Br J Pharmacol. 1995 Mar;114(6):1185-92. doi: 10.1111/j.1476-5381.1995.tb13332.x.

DOI:10.1111/j.1476-5381.1995.tb13332.x

PMID:7620708

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1510338/

Abstract

We investigated the role of angiotensin converting enzyme (ACE) in the cardiovascular effects of N-[1-(R,S)-carboxy-3-phenylpropyl]-Ala-Ala-Tyr-p-aminobenzoate (cFP), a peptidase inhibitor selective for metalloendopeptidase (EP) E.C. 3.4.24.15. 2. In conscious rabbits, cFP (5 mg kg-1, i.v.) markedly slowed the degradation of [3H]-bradykinin, potentiated the depressor response to right atrial administration of bradykinin (10-1000 ng kg-1), and inhibited the pressor response to right atrial angiotensin I (10-100 ng kg-1). In each of these respects, the effects of cFP were indistinguishable from those of the ACE inhibitor, captopril (0.5 mg plus 10 mg kg-1h-1 i.v.). Furthermore, the effects of combined administration of cFP and captopril were indistinguishable from those of captopril alone. 3. In experimentally naive anaesthetized rats, cFP administration (9.3 mg kg-1, i.v.) was followed by a moderate but sustained fall in arterial pressure of 13 mmHg. However, in rats pretreated with bradykinin (50 micrograms kg-1) a more pronounced fall of 30 mmHg was observed. Captopril (5 mg kg-1) had similar hypotensive effects to those of cFP, and cFP had no effect when it was administered after captopril. 4. CFP displaced the binding of [125I]-351A (the p-hydroxybenzamidine derivative of lisinopril) from preparations of rat plasma ACE and solubilized lung membrane ACE (KD = 1.2 and 0.14 microM respectively), and inhibited rat plasma ACE activity (KI = 2.4 microM). Addition of phosphoramidon (10 microM), an inhibitor of a range of metalloendopeptidases, including neutral endopeptidase (E.C.3.4.24.11), markedly reduced the potency of cFP in these systems. 5. Taken together these findings suggest that the actions of cFP in vivo are attributable to inhibition of ACE rather than EP 24.15. Given that cFP is a poor inhibitor of ACE in the presence of phosphoramidon in vitro, it is likely that cFP is cleaved by a phosphoramidon-sensitive metallopeptidase in vivo to liberate N-[1-(R,S)-carboxy-3-phenylpropyl]-Ala-Ala, a potent ACE inhibitor.

摘要

我们研究了血管紧张素转换酶（ACE）在N-[1-(R,S)-羧基-3-苯丙基]-丙氨酰-丙氨酰-酪氨酰-对氨基苯甲酸（cFP）心血管效应中的作用，cFP是一种对金属内肽酶（EP）E.C. 3.4.24.15具有选择性的肽酶抑制剂。2. 在清醒兔中，cFP（5 mg/kg，静脉注射）显著减慢了[3H]-缓激肽的降解，增强了对右心房注射缓激肽（10 - 1000 ng/kg）的降压反应，并抑制了对右心房注射血管紧张素I（10 - 100 ng/kg）的升压反应。在这些方面，cFP的作用与ACE抑制剂卡托普利（0.5 mg加10 mg/kg·h-1，静脉注射）的作用无法区分。此外，cFP和卡托普利联合给药的作用与单独使用卡托普利的作用无法区分。3. 在未经实验处理的麻醉大鼠中，静脉注射cFP（9.3 mg/kg）后，动脉压出现中度但持续的下降，降幅为13 mmHg。然而，在预先用缓激肽（50 μg/kg）处理的大鼠中，观察到更明显的30 mmHg的降幅。卡托普利（5 mg/kg）具有与cFP相似的降压作用，且在卡托普利给药后再给予cFP则无作用。4. cFP使大鼠血浆ACE制剂和溶解的肺膜ACE制剂中[125I]-351A（赖诺普利的对羟基苯甲脒衍生物）的结合发生位移（解离常数分别为1.2和0.14 μM），并抑制大鼠血浆ACE活性（抑制常数为2.4 μM）。加入磷酰胺素（10 μM），一种包括中性内肽酶（E.C.3.4.24.11）在内的多种金属内肽酶的抑制剂，显著降低了cFP在这些系统中的效力。5. 综合这些发现表明，cFP在体内的作用归因于对ACE的抑制而非EP 24.15。鉴于cFP在体外磷酰胺素存在时对ACE的抑制作用较弱，很可能cFP在体内被一种对磷酰胺素敏感的金属肽酶裂解，从而释放出一种强效的ACE抑制剂N-[1-(R,S)-羧基-3-苯丙基]-丙氨酰-丙氨酰。