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钙通道阻滞剂作为血管紧张素I转换酶抑制剂

Calcium channel blockers as inhibitors of angiotensin I-converting enzyme.

作者信息

Casarini D E, Carmona A K, Plavnik F L, Zanella M T, Juliano L, Ribeiro A B

机构信息

Department of Medicine, Escola Paulista de Medicina, Universidade Federal de São Paulo, Brazil.

出版信息

Hypertension. 1995 Dec;26(6 Pt 2):1145-8. doi: 10.1161/01.hyp.26.6.1145.

DOI:10.1161/01.hyp.26.6.1145
PMID:7498985
Abstract

Using ion-exchange chromatography of dialyzed human urine from healthy and hypertensive patients, we detected two peaks of angiotensin I-converting enzyme (ACE) activity on hippuryl-His-Leu eluted at ionic strengths of 0.7 (F1 peak) and 1.25 (F2 peak) mS. These hydrolytic activities decreased gradually in the urine of patients submitted to isradipine treatment, F2 and F1 disappearing after 12 and 24 hours, respectively. By Western blot analysis, the urine fractions corresponding to both peaks from healthy and untreated patients presenting ACE activity and from treated patients (24 hours) without this activity were recognized by an ACE-specific antibody. These results indicated that ACE was present but inhibited in the urine of isradipine-treated patients. In vitro assays with ACE isolated from human urine and guinea pig plasma demonstrated that the enzyme is inhibited by isradipine and other commercially available calcium channel blockers, such as felodipine, nifedipine, and verapamil. A noncompetitive inhibition was observed with all calcium channel blockers studied. In conclusion, these results suggest that besides the primary effect on calcium channels, the more commonly used calcium channel blockers are also ACE inhibitors. The development of efficient calcium channel blockers with higher ACE inhibitory activity could result in interesting bifunctional antihypertensive drugs.

摘要

通过对健康和高血压患者透析后的人尿液进行离子交换色谱分析,我们在离子强度为0.7(F1峰)和1.25(F2峰)mS时洗脱的马尿酰 - 组氨酸 - 亮氨酸上检测到两个血管紧张素I转换酶(ACE)活性峰。在接受伊拉地平治疗的患者尿液中,这些水解活性逐渐降低,F2和F1分别在12小时和24小时后消失。通过蛋白质印迹分析,来自健康和未治疗患者的具有ACE活性的两个峰以及来自无此活性的治疗患者(24小时)的尿液组分被ACE特异性抗体识别。这些结果表明,ACE存在于伊拉地平治疗患者的尿液中但被抑制。用人尿和豚鼠血浆中分离的ACE进行的体外试验表明,该酶被伊拉地平和其他市售钙通道阻滞剂(如非洛地平、硝苯地平和维拉帕米)抑制。在所研究的所有钙通道阻滞剂中均观察到非竞争性抑制作用。总之,这些结果表明,除了对钙通道的主要作用外,常用的钙通道阻滞剂也是ACE抑制剂。开发具有更高ACE抑制活性的高效钙通道阻滞剂可能会产生有趣的双功能抗高血压药物。

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