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氨氯地平每日一次治疗稳定型心绞痛:与安慰剂的双盲交叉对照比较。

Amlodipine once a day in stable angina: double-blind crossover comparison with placebo.

作者信息

Deedwania P C, Cheitlin M D, Das S K, Pool P E, Singh J B, Pasternak R C

机构信息

V.A. Medical Center, Fresno, California.

出版信息

Clin Cardiol. 1993 Aug;16(8):599-602. doi: 10.1002/clc.4960160808.

DOI:10.1002/clc.4960160808
PMID:8370191
Abstract

Although calcium antagonists form a mainstay of therapy in patients with angina pectoris, the currently available agents have significant limitations. Nifedipine, diltiazem, and verapamil are all high-clearance agents with significant hepatic extraction and rapid clearance, leading to limited and short-lived bioavailability necessitating frequent daily administration. In contrast, amlodipine, a dihydropyridine calcium antagonist, has a long half-life of 35-50 h (compared with 3 to 4 h elimination half-life of diltiazem, verapamil, and nifedipine). After oral doses, the relative bioavailability of amlodipine is high (64%) and absorption is smooth, with peak plasma levels being achieved 6-12 h postdose. Bioavailability is not affected by the consumption of food. In common with other dihydropyridine calcium antagonists, amlodipine is eliminated mainly by metabolism. None of the metabolites of amlodipine has significant calcium antagonist effects in humans. In contrast to verapamil or diltiazem, amlodipine has no effect on sinus or atrioventricular node and little or no effect on the resting heart rate. Amlodipine does not have any appreciable negative inotropic effect with the relevant clinical dose. Other clinical studies have shown amlodipine to be effective when used once-daily in chronic stable angina and vasospastic angina. Comparative studies indicate that the antianginal efficacy of amlodipine is comparable to the beta blocker nadolol and the benzothiazepine calcium antagonist diltiazem. Amlodipine has also been found to provide improved antianginal effects when combined to treatment with beta blockers and/or long-acting nitrates. Treatment with amlodipine either as monotherapy or combined with other antianginal therapy for up to 26 weeks shows that efficacy is maintained, with no evidence of tolerance.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

尽管钙拮抗剂是心绞痛患者治疗的主要药物,但目前可用的药物有显著局限性。硝苯地平、地尔硫䓬和维拉帕米都是高清除率药物,有显著的肝脏摄取和快速清除,导致生物利用度有限且持续时间短,需要每日频繁给药。相比之下,二氢吡啶类钙拮抗剂氨氯地平的半衰期长达35 - 50小时(而地尔硫䓬、维拉帕米和硝苯地平的消除半衰期为3至4小时)。口服给药后,氨氯地平的相对生物利用度较高(64%),吸收平稳,给药后6 - 12小时达到血浆峰值水平。生物利用度不受食物摄入的影响。与其他二氢吡啶类钙拮抗剂一样,氨氯地平主要通过代谢消除。氨氯地平的代谢产物在人体中均无显著的钙拮抗作用。与维拉帕米或地尔硫䓬不同,氨氯地平对窦房结或房室结无影响,对静息心率几乎没有影响。在相关临床剂量下,氨氯地平没有任何明显的负性肌力作用。其他临床研究表明,氨氯地平每日一次用于慢性稳定型心绞痛和血管痉挛性心绞痛时有效。比较研究表明,氨氯地平的抗心绞痛疗效与β受体阻滞剂纳多洛尔和苯并噻氮䓬类钙拮抗剂地尔硫䓬相当。还发现氨氯地平与β受体阻滞剂和/或长效硝酸盐联合治疗时能提供更好的抗心绞痛效果。氨氯地平单药治疗或与其他抗心绞痛疗法联合治疗长达26周的结果表明,疗效得以维持,且无耐受性证据。(摘要截选至250字)

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引用本文的文献

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Drug Saf. 1997 Aug;17(2):105-18. doi: 10.2165/00002018-199717020-00003.
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North of England evidence based guidelines development project: summary version of evidence based guideline for the primary care management angina. North of England Stable Angina Guideline Development Group.
英格兰北部循证指南制定项目:初级保健管理心绞痛循证指南概要版。英格兰北部稳定性心绞痛指南制定小组。
BMJ. 1996 Mar 30;312(7034):827-32.
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