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黏菌素与多黏菌素 B 诱导的肾毒性之战

Battle of polymyxin induced nephrotoxicity: Polymyxin B versus colistin.

机构信息

Department of Clinical Pharmacy, Gazi University Faculty of Pharmacy, Ankara, Türkiye; Department of Clinical Pharmacy, Hacettepe University Faculty of Pharmacy, Ankara, Türkiye.

Department of Clinical Pharmacy, Hacettepe University Faculty of Pharmacy, Ankara, Türkiye.

出版信息

Int J Antimicrob Agents. 2024 Feb;63(2):107035. doi: 10.1016/j.ijantimicag.2023.107035. Epub 2023 Nov 17.

Abstract

OBJECTIVES

Nephrotoxicity is the most serious and common adverse effect that limits the use of polymyxins. This study compared polymyxin E (colistin) and polymyxin B regarding drug-related nephrotoxicity.

METHODS

This study was conducted as a retrospective cohort study in a university hospital between January 2020 and July 2022. Patients older than 18 years and who received colistin or polymyxin B were identified using electronic hospital records. Kidney disease improving global outcome criteria were used for assessing nephrotoxicity.

RESULTS

A total of 190 patients, 95 in both groups, were evaluated. The incidence of acute kidney injury during the treatment was higher in the colistin group [52.6% (n = 50) and 34.7% (n = 33), P = 0.013]. In patients who were exposed to high-dose, the rate of nephrotoxicity was higher in patients receiving colistin [25% (n = 3) vs. 76.9% (n = 10); P = 0.017]. Nephrotoxicity was reversible in 64.4% (n = 38) of patients and the reversibility rate was similar (70% and 52.6% for colistin and polymyxin; P = 0.248). In the multivariable analysis, colistin treatment [odds ratio (OR): 3.882, 95% confidence interval (95% CI) = (1.829-8.241)], concomitant vasopressor use (OR = 2.08, CI: 1.036-4.179), and age (OR=1.036, CI: 1.014-1.058) were found to be independent markers of nephrotoxicity.

CONCLUSION

Nephrotoxicity was more common in patients receiving high-dose colistin than polymyxin B. Therefore, the use of appropriate doses of colistin is important in terms of preventing nephrotoxicity. In addition, advancing age and concomitant use of vasopressors contribute to polymyxin-related nephrotoxicity.

摘要

目的

肾毒性是限制多黏菌素使用的最严重和常见的不良反应。本研究比较了黏菌素 E(多黏菌素 E)和黏菌素 B 引起的药物相关性肾毒性。

方法

本研究是在 2020 年 1 月至 2022 年 7 月期间在一所大学医院进行的回顾性队列研究。使用电子病历确定年龄大于 18 岁且接受黏菌素 E 或黏菌素 B 治疗的患者。采用肾脏病改善全球结局标准评估肾毒性。

结果

共评估了 190 例患者,每组 95 例。黏菌素 E 组治疗期间急性肾损伤的发生率较高[52.6%(n=50)和 34.7%(n=33),P=0.013]。在接受高剂量暴露的患者中,接受黏菌素 E 治疗的患者肾毒性发生率较高[25%(n=3)与 76.9%(n=10);P=0.017]。64.4%(n=38)的患者肾毒性可恢复,且恢复率相似(黏菌素 E 组为 70%,黏菌素 B 组为 52.6%;P=0.248)。多变量分析发现,黏菌素 E 治疗[比值比(OR):3.882,95%置信区间(95%CI)(1.829-8.241)]、同时使用血管加压素(OR=2.08,CI:1.036-4.179)和年龄(OR=1.036,CI:1.014-1.058)是肾毒性的独立标志物。

结论

接受高剂量黏菌素 E 治疗的患者比接受黏菌素 B 治疗的患者更常发生肾毒性。因此,在预防肾毒性方面,使用适当剂量的黏菌素 E 非常重要。此外,年龄增长和同时使用血管加压素会导致黏菌素相关性肾毒性。

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