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高血压大鼠中血管紧张素转换酶和中性内肽酶的双重抑制作用

Dual inhibition of angiotensin-converting enzyme and neutral endopeptidase in rats with hypertension.

作者信息

French J F, Anderson B A, Downs T R, Dage R C

机构信息

Marion Merrell Dow Research Institute, Cincinnati, Ohio, USA.

出版信息

J Cardiovasc Pharmacol. 1995 Jul;26(1):107-13. doi: 10.1097/00005344-199507000-00017.

DOI:10.1097/00005344-199507000-00017
PMID:7564349
Abstract

Angiotensin converting enzyme (ACE) and neutral endopeptidase (NEP), are two mechanistically similar enzymes involved in the metabolism of several vasoactive peptides. Selective inhibitors of ACE are effective antihypertensive agents in high-renin, renovascular rats and normal-renin, spontaneously hypertensive rats (SHR), but are not effective in the low-renin, deoxycorticosterone acetate (DOCA)-salt hypertensive rats. In contrast, NEP inhibitors are only effective in the low-renin model of hypertension. Treatment with a combination of selective inhibitors or with a dual inhibitor of both enzymes produces an antihypertensive response regardless of basal plasma renin activity. In this study, we compared the activities of MDL 100,173, a novel subnanomolar inhibitor of both ACE and NEP, with those of equimolar doses of captopril, a selective ACE inhibitor, following intravenous administration in these three rat models of hypertension. Treatment with MDL 100,173 significantly lowered blood pressure compared to vehicle treatment in all three models, whereas captopril treatment lowered blood pressure in the renovascular and SHR models only. Administration of MDL 100,173 also significantly elevated diuresis and natriuresis compared to either vehicle or captopril treatment in the SHR and DOCA-salt rats. Urinary excretion of atrial natriuretic peptide (ANP) was increased by MDL 100,173 treatment in all three models of hypertension. Treatment with captopril did not alter urine, sodium, or ANP excretion in any of the models. However, plasma-renin activity was elevated by both MDL 100,173 and captopril '''''''''''''''''''''''''''''''''''''''''''''''''''''''''''''''''''''''' ''''''''

摘要

血管紧张素转换酶(ACE)和中性内肽酶(NEP)是两种机制相似的酶,参与多种血管活性肽的代谢。ACE的选择性抑制剂在高肾素、肾血管性大鼠以及正常肾素、自发性高血压大鼠(SHR)中是有效的抗高血压药物,但在低肾素、醋酸脱氧皮质酮(DOCA)-盐性高血压大鼠中无效。相比之下,NEP抑制剂仅在低肾素高血压模型中有效。使用选择性抑制剂组合或两种酶的双重抑制剂进行治疗,无论基础血浆肾素活性如何,都会产生抗高血压反应。在本研究中,我们在这三种高血压大鼠模型中静脉注射后,比较了新型亚纳摩尔浓度的ACE和NEP双重抑制剂MDL 100,173与等摩尔剂量的选择性ACE抑制剂卡托普利的活性。与在所有三种模型中给予赋形剂治疗相比,MDL 100,173治疗显著降低了血压,而卡托普利治疗仅在肾血管性和SHR模型中降低了血压。与在SHR和DOCA-盐大鼠中给予赋形剂或卡托普利治疗相比,MDL 100,173给药还显著增加了利尿和利钠作用。在所有三种高血压模型中,MDL 100,173治疗均增加了心房利钠肽(ANP)的尿排泄。卡托普利治疗在任何模型中均未改变尿液、钠或ANP的排泄。然而,MDL 100,173和卡托普利均提高了血浆肾素活性

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