Assessment of prescribed medications and pattern of distribution for potential drug-drug interactions among chronic kidney disease patients attending the Nephrology Clinic of Lagos University Teaching Hospital in Sub-Saharan West Africa.

IF 3.1 Q2 PHARMACOLOGY & PHARMACY Clinical Pharmacology : Advances and Applications Pub Date : 2017-10-26 eCollection Date: 2017-01-01 DOI:10.2147/CPAA.S147835
Olumuyiwa John Fasipe, Peter Ehizokhale Akhideno, Obiyo Nwaiwu, Alex Adedotun Adelosoye
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引用次数: 17

Abstract

Introduction: Life expectancy has increased significantly among chronic kidney disease (CKD) patients due to the extensive use of polypharmacy practice for medication prescriptions. This predisposes them to potential drug-drug interactions (DDIs), which can lead to an increase in morbidity, mortality, length of hospital stay, and health care cost.

Methods: This was a 30-month retrospective study that reviewed the medical case records of consenting adult CKD patients from January 2014 to June 2016. The Medscape drug reference database was used to evaluate patients' medications for potential DDIs.

Results: This study involved 123 adult CKD patients (63 [51.22%] males and 60 [48.78%] females) with a mean age of 53.81±16.03 years. The most common comorbid conditions were hypertension (112 [91.10%]) and diabetes mellitus (45 [36.60%]). Regarding the form of nephrological interventions being offered, the majority of the respondents - 66 (53.66%) were on maintenance dialysis, followed by 53 (43.09%) respondents on conservative care, while 4 (3.25%) respondents were on renal transplantation. A total of 1264 prescriptions were made, and the mean number of prescribed medications per patient was 10.28±3.85. The most frequently prescribed medications were furosemide (88 [71.6%]), heparin (67 [54.47%]), lisinopril (65 [52.9%]), oral calcium carbonate (CaCO3) (63 [51.2%]), α-calcidol (62 [50.4%]), and erythropoietin (61 [49.6%]). A total number of 1851 potential DDIs were observed among 118 patients. The prevalence of potential DDIs in this study was 78.0%, while the mean DDI per prescription was 1.50. Among the potential DDIs observed, the severity was mild in 639 (34.5%) patients, moderate in 1160 (62.7%) patients, and major in 51 (2.8%) patients and only 1 (0.1%) patient was of contraindicated drug combination. The most frequent DDIs' pattern observed was between oral CaCO3 and oral ferrous sulfate. There was a statistically significant association between the number of prescribed medications and the estimated glomerular filtration rate (eGFR; pre-ESRD and ESRD staging) with a P-value of 0.00000119. This implies that the number of prescribed medications increases as the eGFR declines in advance CKD stage patients.

Conclusion: Most of these interactions have moderate severity and delayed onset, hence the need to follow-up these patients after prescription in order to reduce associated morbidity, mortality, length of hospital stay, and health care cost. Physicians and clinical pharmacists should utilise available interaction software to avoid harmful DDIs in these patients.

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西非撒哈拉以南地区拉各斯大学教学医院肾病科门诊慢性肾病患者的处方药物和潜在药物相互作用分布模式评估
由于广泛使用多种药物处方,慢性肾脏疾病(CKD)患者的预期寿命显著增加。这使他们容易发生潜在的药物-药物相互作用(ddi),这可能导致发病率、死亡率、住院时间和医疗保健费用的增加。方法:这是一项为期30个月的回顾性研究,回顾了2014年1月至2016年6月同意的成人CKD患者的医疗病例记录。Medscape药物参考数据库用于评估潜在ddi患者的药物。结果:本研究纳入123例成人CKD患者,其中男性63例[51.22%],女性60例[48.78%],平均年龄53.81±16.03岁。最常见的合并症是高血压(112例[91.10%])和糖尿病(45例[36.60%])。在肾内科干预方式方面,以维持性透析为主,66例(53.66%),保守治疗为主,53例(43.09%),肾移植为主,4例(3.25%)。共开具处方1264张,平均每位患者用药数为10.28±3.85张。常用药物为速尿(88例[71.6%])、肝素(67例[54.47%])、赖诺普利(65例[52.9%])、口服碳酸钙(CaCO3)(63例[51.2%])、α-骨化醇(62例[50.4%])、促红细胞生成素(61例[49.6%])。118例患者共观察到1851个潜在ddi。本研究中潜在DDI的患病率为78.0%,而每张处方的平均DDI为1.50。在观察到的潜在ddi中,轻度639例(34.5%),中度1160例(62.7%),重度51例(2.8%),联合用药禁忌症仅1例(0.1%)。最常见的ddi模式是在口服碳酸钙和口服硫酸亚铁之间。处方药物数量与肾小球滤过率(eGFR;ESRD前期和ESRD分期),p值为0.00000119。这意味着在CKD晚期患者中,处方药物的数量随着eGFR的下降而增加。结论:这些相互作用大多具有中度严重程度和迟发性,因此需要在处方后对这些患者进行随访,以减少相关的发病率、死亡率、住院时间和医疗保健费用。医生和临床药师应利用现有的交互软件来避免这些患者使用有害的ddi。
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CiteScore
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0.00%
发文量
14
审稿时长
16 weeks
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