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用于预防心血管疾病的阿司匹林剂量:一项系统评价。

Aspirin dose for the prevention of cardiovascular disease: a systematic review.

作者信息

Campbell Charles L, Smyth Susan, Montalescot Gilles, Steinhubl Steven R

机构信息

Gill Heart Institute, University of Kentucky, Lexington, USA.

出版信息

JAMA. 2007 May 9;297(18):2018-24. doi: 10.1001/jama.297.18.2018.

DOI:10.1001/jama.297.18.2018
PMID:17488967
Abstract

CONTEXT

More than 50 million US adults take aspirin regularly for long-term prevention of cardiovascular disease, typically either 81 mg/d or 325 mg/d. Controversy remains regarding the most appropriate long-term daily dose.

OBJECTIVE

To review the mechanism of action of aspirin and the clinical literature for relationships among aspirin dosage, efficacy, and safety.

EVIDENCE ACQUISITION

A systematic review of the English-language literature was undertaken using MEDLINE and EMBASE (searched through February 2007) and the search term aspirin or acetylsalicylic acid and dose. The search was limited to clinical trials and was extended by a review of bibliographies of pertinent reports of original data and review articles. Published prospective studies using different aspirin dosages in the setting of cardiovascular disease were included.

EVIDENCE SYNTHESIS

Although pharmacodynamic data demonstrate that long-term aspirin dosages as low as 30 mg/d are adequate to fully inhibit platelet thromboxane production, dosages as high as 1300 mg/d are approved for use. In the United States, 81 mg/d of aspirin is prescribed most commonly (60%), followed by 325 mg/d (35%). The available evidence, predominantly from secondary-prevention observational studies, supports that dosages greater than 75 to 81 mg/d do not enhance efficacy, whereas larger dosages are associated with an increased incidence of bleeding events, primarily related to gastrointestinal tract toxicity.

CONCLUSIONS

Currently available clinical data do not support the routine, long-term use of aspirin dosages greater than 75 to 81 mg/d in the setting of cardiovascular disease prevention. Higher dosages, which may be commonly prescribed, do not better prevent events but are associated with increased risks of gastrointestinal bleeding.

摘要

背景

超过5000万美国成年人长期服用阿司匹林以预防心血管疾病,通常剂量为每日81毫克或325毫克。关于最合适的长期每日剂量仍存在争议。

目的

综述阿司匹林的作用机制以及阿司匹林剂量、疗效和安全性之间关系的临床文献。

证据收集

使用MEDLINE和EMBASE(检索至2007年2月)对英文文献进行系统综述,检索词为阿司匹林或乙酰水杨酸和剂量。检索限于临床试验,并通过查阅原始数据相关报告和综述文章的参考文献进行扩展。纳入了在心血管疾病背景下使用不同阿司匹林剂量的已发表前瞻性研究。

证据综合

尽管药效学数据表明,低至每日30毫克的长期阿司匹林剂量足以完全抑制血小板血栓素生成,但高达每日1300毫克的剂量也被批准使用。在美国,最常开具的阿司匹林剂量是每日81毫克(60%),其次是每日325毫克(35%)。现有证据主要来自二级预防观察性研究,支持大于75至81毫克/天的剂量不会提高疗效,而较大剂量与出血事件发生率增加相关,主要与胃肠道毒性有关。

结论

目前可得的临床数据不支持在预防心血管疾病时常规长期使用大于75至81毫克/天的阿司匹林剂量。可能经常开具的较高剂量并不能更好地预防事件,反而会增加胃肠道出血风险。

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