卡托普利对健康人体中环前列腺素和一氧化氮生成的影响：与低剂量阿司匹林的相互作用。

Effect of captopril on prostacyclin and nitric oxide formation in healthy human subjects: interaction with low dose acetylsalicylic acid.

作者信息

Böger R H, Bode-Böger S M, Kramme P, Tsikas D, Gutzki F M, Frölich J C

机构信息

Institute of Clinical Pharmacology, Medical School, Hannover, Germany.

出版信息

Br J Clin Pharmacol. 1996 Dec;42(6):721-7. doi: 10.1046/j.1365-2125.1996.00480.x.

DOI:10.1046/j.1365-2125.1996.00480.x

PMID:8971427

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2042708/

Abstract

Angiotensin converting enzyme inhibitors have been suggested to act in part by potentiating the stimulatory effect of bradykinin on endothelial prostacyclin and/or nitric oxide (NO) formation. This may give rise to interaction with cyclo-oxygenase inhibiting drugs like acetylsalicylic acid, which is most often used in low doses in patients with cardiovascular diseases. 2. We investigated the effects of captopril (2 x 25 mg day-1), or ASA (1 x 100 mg day-1), or the combination of both drugs for 7 days, on blood pressure, prostanoid and NO formation rates in a double-blind, double dummy, randomized crossover study in 13 healthy female subjects. The urinary metabolites of thromboxane A2 (2,3-dinor-TXB2) and prostacyclin (2,3-dinor-6-keto-PGF1 alpha), and PGE2 were measured by gas chromatography/tandem mass spectrometry in urine on days 1, 6 and 7 of each medication. NO formation was assessed using urinary NO3- and cyclic GMP as indicators. 3. Urinary 2,3-dinor-6-keto-PGF1 alpha excretion was not significantly changed by either captopril, ASA, or their combination. Urinary 2,3-dinor-TXB2 excretion was inhibited by > 80% by ASA alone or in combination with captopril (each P < 0.05), but was not affected by captopril alone. Urinary PGE2 excretion was not significantly changed by either of the treatments. Urinary NO3- and cyclic GMP excretion rates were not significantly changed by captopril, ASA, or their combination. 4. Blood pressure was slightly reduced by captopril. ASA had no effect on blood pressure when given alone, nor did it modulate the effect of captopril on blood pressure during co-administration. Angiotensin II/angiotensin I ratio (index of ACE activity) was significantly decreased by captopril alone or in combination with ASA, but was unaffected by ASA alone. 5. Captopril does not stimulate prostacyclin formation in healthy human subjects in a dose sufficient to substantially inhibit ACE activity. Co-administration of ASA significantly inhibits 2,3-dinor-TXB2 excretion, but does not interfere with the blood pressure lowering effect of captopril in healthy human subjects.

摘要

有研究表明，血管紧张素转换酶抑制剂的部分作用机制是增强缓激肽对内皮前列环素和/或一氧化氮（NO）生成的刺激作用。这可能会导致与环氧化酶抑制药物（如乙酰水杨酸）产生相互作用，而乙酰水杨酸在心血管疾病患者中通常以低剂量使用。2. 我们在13名健康女性受试者中进行了一项双盲、双模拟、随机交叉研究，调查了卡托普利（2×25毫克/天）、阿司匹林（1×100毫克/天）或两种药物联合使用7天对血压、前列腺素和NO生成率的影响。在每种药物治疗的第1天、第6天和第7天，通过气相色谱/串联质谱法测定尿液中血栓素A2（2,3-二去甲血栓素B2）、前列环素（2,3-二去甲-6-酮-前列腺素F1α）和前列腺素E2的尿代谢产物。使用尿硝酸盐和环鸟苷酸作为指标评估NO生成。3. 卡托普利、阿司匹林或它们的组合均未显著改变尿2,3-二去甲-6-酮-前列腺素F1α的排泄。单独使用阿司匹林或与卡托普利联合使用时，尿2,3-二去甲血栓素B2的排泄被抑制>80%（各P<0.05），但单独使用卡托普利时无此影响。两种治疗方法均未显著改变尿前列腺素E2的排泄。卡托普利、阿司匹林或它们的组合均未显著改变尿硝酸盐和环鸟苷酸的排泄率。4. 卡托普利使血压略有降低。单独使用阿司匹林对血压无影响，在联合给药期间也未调节卡托普利对血压的作用。单独使用卡托普利或与阿司匹林联合使用时，血管紧张素II/血管紧张素I比值（ACE活性指标）显著降低，但单独使用阿司匹林时无此影响。5. 卡托普利在足以显著抑制ACE活性的剂量下，不会刺激健康人体受试者中前列环素的生成。联合使用阿司匹林可显著抑制2,3-二去甲血栓素B2的排泄，但不干扰卡托普利在健康人体受试者中的降压作用。