Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.
Pain Pract. 2011 Jul-Aug;11(4):325-36. doi: 10.1111/j.1533-2500.2010.00438.x. Epub 2010 Dec 28.
Patients taking more than one drug metabolized through the cytochrome P450 (CYP450) enzyme system experience a drug-drug exposure (DDE), which puts them at risk for a potential pharmacokinetic drug-drug interaction (DDI), defined as two or more drugs interacting in such a way that the effectiveness and/or toxicity of one or all drugs are changed. Any patient subjected to a DDE is at risk for a potentially serious DDI, the epidemiology of which has not been thoroughly studied. Many drugs are metabolized primarily via the CYP450 enzyme system, including certain opioids used to manage moderate to severe chronic pain. We conducted a retrospective analysis of a large commercial claims database and a Medicare database to assess the prevalence of DDEs among patients with osteoarthritis taking CYP450-metabolized opioids. The overall prevalence of DDEs in this population was 26%, with females more likely to experience DDEs than males (28.4% vs. 21.0%, respectively). The number of unique concurrent prescriptions at baseline, gender, age, and Charlson Comorbidity Index were statistically significant predictors of DDEs (P < 0.05). This study challenged previous assumptions about DDEs in that advanced age was not positively associated with the risk of DDE. However, the number of prescriptions the patient received in the 90-day window prior to the index date was a risk factor. For patients taking at least two medications in the 90-day period prior to the index date, every additional prescription taken increased their risk for a DDE during the observation period by 138% (on average). The risk of DDE during the study period was threefold greater for patients with one medication in the 90-day period before index date compared with similar patients with no prescriptions in that same period before the index date. DDEs are more common than may be generally believed in patients with osteoarthritis, regardless of age, and can occur even in patients taking few medications. When selecting an opioid analgesic to treat osteoarthritis, physicians should consider the potential for exposure of these patients to drugs that could interact unfavorably.
患者同时服用多种经细胞色素 P450(CYP450)酶系统代谢的药物时,会发生药物-药物暴露(DDE),这使他们面临潜在的药代动力学药物-药物相互作用(DDI)的风险,定义为两种或多种药物以相互作用的方式,使一种或所有药物的有效性和/或毒性发生变化。任何接受 DDE 的患者都有发生潜在严重 DDI 的风险,但其流行病学尚未得到充分研究。许多药物主要通过 CYP450 酶系统代谢,包括某些用于治疗中重度慢性疼痛的阿片类药物。我们对大型商业索赔数据库和医疗保险数据库进行了回顾性分析,以评估服用 CYP450 代谢阿片类药物的骨关节炎患者中 DDE 的发生率。该人群中 DDE 的总体发生率为 26%,女性发生 DDE 的可能性高于男性(分别为 28.4%和 21.0%)。基线时的独特同时处方数量、性别、年龄和 Charlson 合并症指数是 DDE 的统计学显著预测因素(P<0.05)。这项研究挑战了之前关于 DDE 的假设,即高龄与 DDE 风险没有正相关。然而,患者在索引日期前 90 天内收到的处方数量是一个风险因素。对于在索引日期前 90 天内至少服用两种药物的患者,在观察期间,每增加一种处方,其发生 DDE 的风险就会增加 138%(平均)。与索引日期前 90 天内无处方的类似患者相比,索引日期前 90 天内服用一种药物的患者在研究期间发生 DDE 的风险高 3 倍。无论年龄大小,骨关节炎患者中的 DDE 比普遍认为的更为常见,即使是服用少量药物的患者也可能发生 DDE。在选择阿片类镇痛药治疗骨关节炎时,医生应考虑到这些患者可能会接触到可能产生不利相互作用的药物。
Zotero 插件