佐非诺普利和雷米普利对健康志愿者咳嗽反射和气道炎症的交叉随机对照研究。

Cough (London, England) Pub Date : 2014-12-24 eCollection Date: 2014-01-01 DOI:10.1186/s12997-014-0007-5
Federico Lavorini, Elisa Chellini, Margherita Innocenti, Giacomo Campi, Colin Gerard Egan, Selene Mogavero, Giovanni A Fontana
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引用次数: 7

摘要

背景:持续干咳是众所周知的血管紧张素转换酶抑制剂(ACE-i)的不良反应。动物研究表明,与广泛使用的ACE-i雷米普利相比,ACE-i唑非普利的致病菌效应更小。本研究的目的是比较健康志愿者对吸入性tussigens的咳嗽敏感性,以及服用唑非诺普利和雷米普利后自发性咳嗽的情况;同时收集了唑非诺普利和雷米普利的药代动力学(PK)数据,以及它们各自的活性形态,唑非诺普利和雷米普利。方法:40名健康志愿者加入随机交叉研究。患者分别给予佐非那普利钙盐(试验药物)包衣片30 mg /日或雷米普利(参比药物)片10 mg /日,连续7 d,分两期服用,中间间隔21 d洗脱期。对辣椒素和柠檬酸的咳嗽敏感性被评估为引起至少2次(C2)或5次咳嗽(C5)的每一种咳嗽剂的浓度;在整个研究过程中也对自发性咳嗽进行了监测。在两个研究时段分别采集唑非诺普利、雷米普利及其活性形态的PK参数。通过呼气一氧化氮分数(FeNO)和缓激肽(BK)水平评估气道炎症,在每个治疗期之前和之后测量。结论:与雷米普利相比,左非普利的促炎活性降低,对咳嗽反射的影响更小,这表明左非普利更有利。
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A crossover randomized comparative study of zofenopril and ramipril on cough reflex and airway inflammation in healthy volunteers.

Background: Persistent dry cough is a well known unwanted effect of Angiotensin-Converting Enzyme inhibitors (ACE-i). Animal studies have shown that the ACE-i zofenopril has a less tussigenic effect compared to the widely used ACE-i ramipril. The aim of this study was to compare cough sensitivity to inhaled tussigens, as well as spontaneous cough in response to the administration of zofenopril and ramipril in healthy volunteers; pharmacokinetic (PK) data of both zofenopril and ramipril, as well as their respective active forms, zofenoprilat and ramiprilat, was also collected.

Methods: Forty healthy volunteers were enrolled in a randomized crossover study. Patients were administered zofenopril calcium salt (test drug) coated tablets, 30 mg daily dose or ramipril (reference drug) tablets, 10 mg daily dose, for 7 consecutive days in two periods separated by a 21-day wash-out period. Cough sensitivity to capsaicin and citric acid was assessed as the concentration of each tussigenic agent causing at least 2 (C2) or 5 coughs (C5); spontaneous cough was also monitored throughout the study. PK parameters of zofenopril, ramipril and their active forms, were collected for each of the two study periods. Airway inflammation, as assessed by fractional exhaled nitric oxide (FeNO) and bradykinin (BK) levels, were measured prior to and following each treatment period.

Results: Ramipril, but not zofenopril, increased (p < 0.01) cough sensitivity to both tussigenic agents as assessed by C2. With citric acid, C5 values calculated after both ramipril and zofenopril administration were significantly (p < 0.05 and p < 0.01, respectively) lower than corresponding control values. With both ACE-i drugs, spontaneous cough was infrequently reported by subjects. Zofenopril/zofenoprilat PK analysis showed higher area under the curve of plasma concentration, τ values (ng/ml x h) than ramipril/ramiprilat (zofenopril vs. ramipril, 84.25 ± 34.47 vs. 47.40 ± 21.30; and zofenoprilat vs. ramiprilat, 653.67 ± 174.91 vs. 182.26 ± 61.28). Both ACE-i drugs did not affect BK plasma levels; in contrast, ramipril, but not zofenopril, significantly increased control FeNO values (from 24 ± 9.6 parts per billion [PPB] to 33 ± 16 PPB; p < 0.01).

Conclusions: Zofenopril has a more favourable profile when compared to ramipril as shown by a reduced pro-inflammatory activity and less impact on the cough reflex.

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A crossover randomized comparative study of zofenopril and ramipril on cough reflex and airway inflammation in healthy volunteers. Standardized method for solubility and storage of capsaicin-based solutions for cough induction. On the definition of chronic cough and current treatment pathways: an international qualitative study. Effect of acid suppression therapy on gastroesophageal reflux and cough in idiopathic pulmonary fibrosis: an intervention study. Severity of cough in idiopathic pulmonary fibrosis is associated with MUC5 B genotype.
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