Abdulwasiu Adeniyi Busari, Ibrahim A Oreagba, Kazeem A Oshikoya, Mary O Kayode, Sunday O Olayemi
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引用次数: 4
Abstract
Background: Potential drug-drug interactions (DDIs) are increasingly common in clinical practice, especially among individuals with chronic conditions, such as chronic kidney dysfunction. However, data relating to DDIs among chronically ill patients are limited in Nigeria. We, therefore, investigated the prevalence and pattern of DDIs among patients with kidney diseases on admission at a tertiary hospital in Lagos, Nigeria.
Materials and methods: This was a prospective observational study involving 61 adults with kidney diseases and on admission in medical wards of the study center, over a 3-month period. Data extractions were with a purposefully designed pro forma to extract relevant data on demographic, clinical, and dosing regimens of the prescribed drugs for individual patients. Potential DDIs were identified, and their severity was rated using the MICROMEDEX® software database (IBM® Watson-Truven Health Analytics), which is available online with limited access.
Results: Of the 61 patients evaluated, majority were males (34; 55.7%), were elderly (26; 42.6%), and had chronic kidney disease Stage 3 (40; 65.5%). The most common cause of kidney disease was hypertension (20; 32.8%). Out of the 542 prescriptions received by the patients, potential DDI was observed in 508 (93.7%) prescriptions. Clinically significant drug interactions (CSDIs) were detected in 486 (85.7%) prescriptions. Pharmacodynamic DDIs (466; 91.7%) were the most common. Pill burden exceeding 25 pills/day was present in nine (14.8%) patients. The severities of the potential DDIs were major (135; 24.9%), moderate (333; 61.4%), and minor (38; 7.1%). Only two different potential DDIs were rated X (contraindicated).
Conclusion: Exposure to drugs with potential DDIs was very common among patients with kidney diseases. Most of the CSDIs observed were of major severity. The use of DDI checker before prescribing drugs for individuals with kidney diseases could avert clinically significant interactions.
背景:潜在的药物-药物相互作用(ddi)在临床实践中越来越普遍,特别是在慢性疾病,如慢性肾功能不全的个体中。然而,在尼日利亚,与慢性病患者的DDIs有关的数据有限。因此,我们调查了尼日利亚拉各斯一家三级医院住院的肾病患者ddi的患病率和模式。材料和方法:这是一项前瞻性观察性研究,涉及61名患有肾脏疾病的成年人,并在研究中心的内科病房入院,为期3个月。数据提取采用有目的设计的形式,以提取个体患者的人口统计学、临床和处方药物给药方案的相关数据。确定潜在的ddi,并使用MICROMEDEX®软件数据库(IBM®Watson-Truven Health Analytics)对其严重程度进行评级,该数据库可在线获得,但访问权限有限。结果:61例患者中,男性居多(34例;55.7%),老年人(26例;42.6%),并且患有慢性肾脏疾病3期(40;65.5%)。肾脏疾病最常见的原因是高血压(20;32.8%)。542张处方中,508张(93.7%)处方存在潜在DDI。486张(85.7%)处方中存在临床显著药物相互作用(csdi)。药效学ddi (466;91.7%)是最常见的。9例(14.8%)患者的服药负担超过25片/天。潜在ddi的严重程度主要(135例;24.9%),中等(333;61.4%),未成年人(38%;7.1%)。只有两个不同的潜在ddi被评为X级(禁忌)。结论:潜在ddi药物暴露在肾脏疾病患者中非常普遍。大多数观察到的csdi都是严重的。肾脏疾病患者在开药前使用DDI检测仪可以避免临床显著的相互作用。