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双氯芬酸剂量与胃肠道及心血管事件风险之间的关系:基于两项系统文献综述的Meta回归分析

Relationship between diclofenac dose and risk of gastrointestinal and cardiovascular events: meta-regression based on two systematic literature reviews.

作者信息

Odom Dawn M, Mladsi Deirdre M, Saag Kenneth G, Sherif Bintu N, Miles LaStella, Ronquest Naoko, Wang Jianmin

机构信息

RTI Health Solutions, Research Triangle Park, North Carolina.

RTI Health Solutions, Research Triangle Park, North Carolina.

出版信息

Clin Ther. 2014 Jun 1;36(6):906-17. doi: 10.1016/j.clinthera.2014.04.012. Epub 2014 May 23.

Abstract

BACKGROUND

NSAIDs are associated with risks of gastrointestinal (GI) and cardiovascular (CV) toxicities. It has been reported that the risks of GI and CV events are dose related, resulting in guidance explicitly emphasizing the use of NSAIDs at the lowest effective dose for the shortest duration. To understand the potential benefits of using lower doses of diclofenac, a more detailed understanding of the relationship of diclofenac dose and the risks of GI and CV events is required.

OBJECTIVE

The objective of this study was to extend previous research quantifying the NSAID dose-toxicity relationship by modeling dose as a continuous measure, allowing for an assessment of the risks of major GI and CV events for patients taking specific diclofenac doses compared with NSAID nonusers.

METHODS

We used studies identified in 2 recently published systematic reviews of observational studies that examined the risks of major GI and CV events associated with the use of oral NSAIDs. We developed meta-regression models, considering dose as a continuous measure, to estimate the risks of major GI and CV events for different daily doses of conventional oral diclofenac relative to nonuse of NSAIDs.

RESULTS

Seven of the 59 GI publications, contributing 11 dose-specific risk ratio observations, and 12 of the 51 CV studies, contributing 21 dose-specific risk ratio observations, were eligible for inclusion in the meta-regression. The models indicated positive linear relationships between diclofenac dose and the relative risks of major GI and CV events for the range of doses examined.

CONCLUSIONS

To our knowledge, this is the first study to quantify and aggregate the continuous relationship between the risk of GI or CV events and the dosage of an NSAID. With the recent availability of new low doses of diclofenac, the models may be used to estimate the potential reduction in risk of adverse events at these doses.

摘要

背景

非甾体抗炎药(NSAIDs)与胃肠道(GI)和心血管(CV)毒性风险相关。据报道,胃肠道和心血管事件的风险与剂量相关,这导致相关指南明确强调应使用最低有效剂量的NSAIDs,并尽可能缩短用药时间。为了解使用较低剂量双氯芬酸的潜在益处,需要更详细地了解双氯芬酸剂量与胃肠道和心血管事件风险之间的关系。

目的

本研究的目的是通过将剂量建模为连续变量来扩展先前关于NSAIDs剂量-毒性关系量化的研究,从而能够评估服用特定双氯芬酸剂量的患者与未使用NSAIDs的患者相比发生主要胃肠道和心血管事件的风险。

方法

我们使用了最近发表的2篇观察性研究系统评价中确定的研究,这些研究考察了口服NSAIDs相关的主要胃肠道和心血管事件风险。我们开发了元回归模型,将剂量视为连续变量,以估计相对于未使用NSAIDs,不同日剂量的传统口服双氯芬酸发生主要胃肠道和心血管事件的风险。

结果

59篇胃肠道相关出版物中的7篇(提供了11个剂量特异性风险比观察值)以及51篇心血管相关研究中的12篇(提供了21个剂量特异性风险比观察值)符合纳入元回归的条件。模型表明,在所研究的剂量范围内,双氯芬酸剂量与主要胃肠道和心血管事件的相对风险之间存在正线性关系。

结论

据我们所知,这是第一项量化并汇总胃肠道或心血管事件风险与NSAIDs剂量之间连续关系的研究。随着近期新的低剂量双氯芬酸的出现,这些模型可用于估计这些剂量下不良事件风险的潜在降低情况。

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