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有癌症病史患者的潜在药物相互作用。

Potential drug interactions in patients with a history of cancer.

机构信息

University of British Columbia, Vancouver, BC.

University of British Columbia, Vancouver, BC. ; Division of Medical Oncology, BC Cancer Agency, Vancouver, BC.

出版信息

Curr Oncol. 2014 Apr;21(2):e212-20. doi: 10.3747/co.21.1657.

Abstract

BACKGROUND

Cancer survivors (css) are frequently exposed to polypharmacy, which might increase their risk of drug interactions. Our study aimed to determine the relative prevalence of potential drug interactions (pdis) among css compared with non-cancer respondents (ncrs).

METHODS

Self-reported prescription data from 4975 patients were extracted from the U.S. National Health and Nutrition Examination Survey and screened for pdis using iFacts: Drug Interaction Facts (Facts and Comparisons, St. Louis, MO, U.S.A.). The clinical significance of each pdi was graded on a 5-point scale based on the severity of the interaction and the level of evidence documenting the interaction. Summary statistics and logistic regression models were used to assess the impact of cancer history on the risk of pdis.

RESULTS

Of patients eligible for the analyses, the css (n = 302) indicated using 4.4 ± 0.22 prescriptions on average, and the ncrs (n = 908), 3.8 ± 0.09. Nearly half of both cohorts (40% of css, 43% of ncrs) had at least 1 pdi. In both cohorts, 12% were at risk for fatal or permanently debilitating effects. In multivariate analyses, css were significantly less likely than ncrs to be at risk for any pdis (odds ratio: 0.65; 95% confidence interval: 0.46 to 0.92; p = 0.02). Advanced age and low household income were associated with pdis among css. Medications most commonly prescribed to css with a pdi included metoprolol (15.6%), levothyroxine (13.6%), and furosemide (11.9%).

CONCLUSIONS

Although css appear to be less susceptible than ncrs to pdis, the prevalence of pdis among css remains suboptimal. Specific subgroups of css may be particularly prone to pdis, underscoring the importance of increased vigilance.

摘要

背景

癌症幸存者(css)经常面临多种药物治疗,这可能会增加他们发生药物相互作用的风险。我们的研究旨在确定与非癌症对照者(ncrs)相比,css 发生潜在药物相互作用(pdi)的相对流行率。

方法

从美国国家健康和营养检查调查中提取了 4975 名患者的自我报告处方数据,并使用 iFacts:药物相互作用事实(事实和比较,密苏里州圣路易斯,美国)筛选 pdi。根据相互作用的严重程度和记录相互作用的证据水平,对每个 pdi 的临床意义进行 5 分制评分。使用汇总统计和逻辑回归模型评估癌症病史对 pdi 风险的影响。

结果

在符合分析条件的患者中,css(n=302)平均使用 4.4±0.22 种处方,ncrs(n=908)平均使用 3.8±0.09 种处方。两个队列的近一半(css 组 40%,ncrs 组 43%)至少有一种 pdi。在两个队列中,都有 12%的患者有发生致命或永久性致残作用的风险。在多变量分析中,css 发生任何 pdi 的风险显著低于 ncrs(比值比:0.65;95%置信区间:0.46 至 0.92;p=0.02)。年龄较大和家庭收入较低与 css 发生 pdi 相关。在有 pdi 的 css 中最常开的药物包括美托洛尔(15.6%)、左甲状腺素(13.6%)和呋塞米(11.9%)。

结论

尽管 css 似乎比 ncrs 不易发生 pdi,但 css 中 pdi 的流行率仍不理想。css 的特定亚组可能特别容易发生 pdi,这凸显了提高警惕的重要性。

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