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预防非甾体抗炎药的胃肠道不良反应:从危险因素识别到危险因素干预。

Preventing the gastrointestinal adverse effects of nonsteroidal anti-inflammatory drugs: from risk factor identification to risk factor intervention.

机构信息

Inserm CIC-P 803, CHU de Dijon, 1, boulevard Jeanne-d'Arc, BP 1542, 21000 Dijon, France.

出版信息

Joint Bone Spine. 2010 Jan;77(1):6-12. doi: 10.1016/j.jbspin.2009.11.008. Epub 2009 Dec 21.

Abstract

Nonsteroidal anti-inflammatory drugs (NSAIDs) have huge prescription volumes, for two main reasons: the aging of the population is increasing the prevalence of diseases that respond to NSAIDs, such as osteoarthritis; and NSAIDs are highly effective drugs that contribute crucially to the management of many diseases. In France, the number of physician orders that include an NSAID is estimated at 25 to 30 million per year. Nevertheless, the use of NSAIDs is limited by adverse effects. The gastrointestinal tract is the main target of NSAID toxicity, and NSAID therapy is among the leading causes of bleeding from upper gastrointestinal ulcers. Adverse events targeting the lower gastrointestinal tract are also of concern, although they receive less attention. To effectively prevent NSAID toxicity, it must be recognized that the risk of adverse events can be diminished but not eliminated. Therefore, the risk/benefit ratio must be carefully evaluated at each prescription. A number of risk factors should be emphasized. Thus, the risk increases with age, and there is a sharp risk increase at 60 years of age. Other risk factors include a history of ulcers (most notably with bleeding), the use of high NSAID dosages, Helicobacter pylori infection, and the concomitant use of antiplatelet agents. Minimizing NSAID-related gastrointestinal toxicity requires a careful risk factor evaluation; selection of the most appropriate NSAID and NSAID dosage; and, in some patients, prophylactic gastroprotective therapy, for instance with a proton pump inhibitor. Gastrointestinal symptoms either have no value for predicting gastrointestinal events or occur too late to serve as alarm signals. The toxicity advantages of cyclooxygenase-2 inhibitors seem modest and do not eliminate the need for this rational prescription strategy.

摘要

非甾体抗炎药(NSAIDs)的处方量巨大,主要有两个原因:人口老龄化导致对 NSAIDs 有反应的疾病(如骨关节炎)的患病率增加;而且 NSAIDs 是非常有效的药物,对许多疾病的治疗至关重要。在法国,每年包含 NSAID 的医生处方数量估计为 2500 万至 3000 万张。然而,NSAIDs 的使用受到不良反应的限制。胃肠道是 NSAID 毒性的主要靶标,NSAID 治疗是上消化道溃疡出血的主要原因之一。下消化道靶向的不良反应也值得关注,尽管它们受到的关注较少。为了有效预防 NSAID 毒性,必须认识到不良反应的风险可以降低但不能消除。因此,在每次处方时都必须仔细评估风险/效益比。有几个危险因素需要强调。因此,风险随着年龄的增长而增加,60 岁时风险急剧增加。其他危险因素包括溃疡史(尤其是出血性溃疡)、高剂量 NSAID 使用、幽门螺杆菌感染和抗血小板药物的同时使用。最大限度地减少 NSAID 相关的胃肠道毒性需要仔细评估危险因素;选择最合适的 NSAID 和 NSAID 剂量;在某些患者中,预防性胃保护治疗,例如质子泵抑制剂。胃肠道症状对于预测胃肠道事件没有价值,或者发生得太晚,无法作为警报信号。环氧化酶-2 抑制剂的毒性优势似乎微不足道,并且不能消除这种合理的处方策略的必要性。

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