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果阿医学院住院患者因多种药物联合使用导致的有害药物相互作用研究。

A study of harmful drug-drug interactions due to polypharmacy in hospitalized patients in Goa Medical College.

作者信息

Khandeparkar Akshay, Rataboli Padmanabh V

机构信息

Department of Medical Affairs, Roche Pharmaceuticals, Mumbai, Maharashtra, India.

Department of Pharmacology, Goa Medical College, Goa, India.

出版信息

Perspect Clin Res. 2017 Oct-Dec;8(4):180-186. doi: 10.4103/picr.PICR_132_16.

Abstract

INTRODUCTION

Concomitant use of multiple drugs is often indicated to manage comorbid conditions and enhance efficacy. Such concomitant use of multiple drugs (five or more drugs) has been defined as "polypharmacy." Polypharmacy has been associated with adverse consequences such as greater healthcare costs, increased risk of adverse drug events, drug-drug interactions (DDIs), medication nonadherence, reduced functional capacity, and multiple geriatric syndromes. This study evaluated number of potential harmful DDIs due to polypharmacy.

MATERIALS AND METHODS

A prospective, cross-sectional, observational study was performed from July 2011 to June 2012. Approval was obtained from the Institutional Ethics Committee, Goa Medical College. Drug interactions were identified using a computerized DDI database system Lexi-Comp version: 2.4.1. Quantitative data analysis was done by the SPSS for Windows version 17.0.

RESULTS

Seven hundred and fifty-one out of 5424 (13.85%) prescriptions were observed to have polypharmacy with highest rates observed in the Department of Medicine. The median age of patients was 55.60 ± 13.86 (range 10-108 years). A total number of drugs per prescription ranged from minimum of 5 to maximum of 16 drugs, with an average of 7.96 ± 1.75. A large number of 596 prescriptions contained 6-9 drugs per prescription. Drugs involved in potential DDIs in our study included aspirin, antacids, beta-blockers, 3-hydroxy-3-methylglutaryl-coenzyme reductase inhibitors, calcium channel blockers, angiotensin-converting enzyme inhibitors, ondansetron, and H2 blockers.

CONCLUSION

Patients taking multiple medications experience unique pharmacotherapy. Personalized drug prescribing strategies and close monitoring of patients taking drugs with potential DDIs are keys to optimal therapeutic result.

摘要

引言

为控制共病情况并提高疗效,常需联合使用多种药物。这种联合使用多种药物(五种或更多药物)的情况被定义为“多重用药”。多重用药与诸多不良后果相关,如更高的医疗成本、药物不良事件风险增加、药物相互作用(DDIs)、用药依从性降低、功能能力下降以及多种老年综合征。本研究评估了多重用药导致的潜在有害药物相互作用的数量。

材料与方法

2011年7月至2012年6月进行了一项前瞻性、横断面观察性研究。获得了果阿医学院机构伦理委员会的批准。使用计算机化的药物相互作用数据库系统Lexi-Comp版本2.4.1识别药物相互作用。通过SPSS for Windows版本17.0进行定量数据分析。

结果

在5424份处方中,有751份(13.85%)存在多重用药情况,其中内科的发生率最高。患者的中位年龄为55.60±13.86岁(范围10 - 108岁)。每份处方的药物总数最少为5种,最多为16种,平均为7.96±1.75种。大量的596份处方每份含有6 - 9种药物。我们研究中涉及潜在药物相互作用的药物包括阿司匹林、抗酸剂、β受体阻滞剂、3 - 羟基 - 3 - 甲基戊二酰辅酶A还原酶抑制剂、钙通道阻滞剂、血管紧张素转换酶抑制剂、昂丹司琼和H2受体阻滞剂。

结论

服用多种药物的患者经历独特的药物治疗。个性化的药物处方策略以及对服用可能存在药物相互作用药物的患者进行密切监测是实现最佳治疗效果的关键。

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