中性内肽酶的抑制在体内会导致人体阻力血管收缩。

Inhibition of neutral endopeptidase causes vasoconstriction of human resistance vessels in vivo.

作者信息

Ferro C J, Spratt J C, Haynes W G, Webb D J

机构信息

Clinical Pharmacology Unit and Research Centre, University of Edinburgh, Western General Hospital, UK.

出版信息

Circulation. 1998 Jun 16;97(23):2323-30. doi: 10.1161/01.cir.97.23.2323.

DOI:10.1161/01.cir.97.23.2323

PMID:9639376

Abstract

BACKGROUND

Neutral endopeptidase (NEP) degrades vasoactive peptides, including the natriuretic peptides, angiotensin II, and endothelin-1. Systemic inhibition of NEP does not consistently lower blood pressure, even though it increases natriuretic peptide concentrations and causes natriuresis and diuresis. We therefore investigated the direct effects of local inhibition of NEP on forearm resistance vessel tone.

METHODS AND RESULTS

Four separate studies were performed, each with 90-minute drug infusions. In the first study, 10 healthy subjects received a brachial artery infusion of the NEP inhibitor candoxatrilat (125 nmol/min), which caused a slowly progressive forearm vasoconstriction (12+/-2%; P=0.001). In a second two-phase study, 6 healthy subjects received, 4 hours after enalapril (20 mg) or placebo, an intra-arterial infusion of the NEP inhibitor thiorphan (30 nmol/min). Thiorphan caused similar degrees of local forearm vasoconstriction (P=0.6) after pretreatment with both placebo (13+/-1%, P=0.006) and enalapril (17+/-6%, P=0.05). In a third three-phase study, 8 healthy subjects received intra-arterial thiorphan (30 nmol/min), the endothelin ETA antagonist BQ-123 (100 nmol/min), and both combined. Thiorphan caused local forearm vasoconstriction (13+/-1%, P=0.0001); BQ-123 caused local vasodilatation (33+/-3%, P=0.0001). Combined thiorphan and BQ-123 caused vasodilatation (32+/-1%, P=0.0001) similar to BQ-123 alone (P=0.98). In a fourth study, 6 hypertensive patients (blood pressure >160/100 mm Hg) received intra-arterial thiorphan (30 nmol/min). Thiorphan caused a slowly progressive forearm vasoconstriction (10+/-2%, P=0.0001).

CONCLUSIONS

Inhibition of local NEP causes vasoconstriction in forearm resistance vessels of both healthy volunteers and patients with hypertension. The lack of effect of ACE inhibition on the vasoconstriction produced by thiorphan and its absence during concomitant ETA receptor blockade suggest that it is mediated by endothelin-1 and not angiotensin II. These findings may help to explain the failure of systemic NEP inhibition to lower blood pressure.

摘要

背景

中性内肽酶（NEP）可降解血管活性肽，包括利钠肽、血管紧张素II和内皮素-1。尽管抑制NEP可增加利钠肽浓度并导致利钠和利尿，但对其进行全身抑制并不能持续降低血压。因此，我们研究了局部抑制NEP对前臂阻力血管张力的直接影响。

方法与结果

进行了四项独立研究，每项研究均进行90分钟的药物输注。在第一项研究中，10名健康受试者接受肱动脉输注NEP抑制剂坎多沙坦酯（125 nmol/分钟），这导致前臂缓慢进行性血管收缩（12±2%；P=0.001）。在第二项两阶段研究中，6名健康受试者在服用依那普利（20 mg）或安慰剂4小时后，接受动脉内输注NEP抑制剂硫磷酰胺（30 nmol/分钟）。在接受安慰剂（13±1%，P=0.006）和依那普利（17±6%，P=0.05）预处理后，硫磷酰胺引起的局部前臂血管收缩程度相似（P=0.6）。在第三项三阶段研究中，8名健康受试者接受动脉内硫磷酰胺（30 nmol/分钟）、内皮素ETA拮抗剂BQ-123（100 nmol/分钟）以及两者联合使用。硫磷酰胺引起局部前臂血管收缩（13±1%，P=0.0001）；BQ-123引起局部血管舒张（33±3%，P=0.0001）。硫磷酰胺和BQ-123联合使用引起的血管舒张（32±1%，P=0.0001）与单独使用BQ-123相似（P=0.98）。在第四项研究中，6名高血压患者（血压>160/100 mmHg）接受动脉内硫磷酰胺（30 nmol/分钟）。硫磷酰胺引起前臂缓慢进行性血管收缩（10±2%，P=0.0001）。