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Development of acute kidney injury during continuous infusion of vancomycin in septic patients

机译:脓毒症患者持续输注万古霉素期间发生急性肾损伤

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Purpose: Few data are available on the occurrence of renal failure during continuous infusion of vancomycin in critically ill patients. Methods: We reviewed the data of all patients admitted to the intensive care unit (ICU) between January 2008 and December 2009 in whom vancomycin was given as a continuous infusion for more than 48 h in the absence of renal replacement therapy. We collected data on the doses of vancomycin and blood concentrations during therapy. Acute kidney injury (AKI) was defined as a daily urine output 0.5 ml/kg/h and/or an increase in the serum creatinine of ≥0.3 mg/dl from baseline levels during vancomycin therapy or within 72 h after its discontinuation. Multivariable logistic regression analysis was performed to identify predictors of AKI. Results: Of 207 patients who met the inclusion criteria, 50 (24 %) developed AKI. These patients were more severely ill, had lower creatinine clearance at admission, were more frequently exposed to other nephrotoxic agents, had a longer duration of therapy, and had higher concentrations of vancomycin during the first 3 days of treatment (C mean). The C mean was independently associated with early AKI (within 48 h from the onset of therapy) and the duration of vancomycin administration with late AKI. Conclusions: AKI occurred in almost 25 % of critically ill patients treated with a continuous infusion of vancomycin. Vancomycin concentrations and duration of therapy were the strongest variables associated with the development of early and late AKI during therapy, respectively.
机译:目的:在危重病人连续输注万古霉素期间发生肾衰竭的数据很少。方法:我们回顾了2008年1月至2009年12月在重症监护病房(ICU)住院的所有患者的数据,这些患者在不进行肾脏替代疗法的情况下连续输注万古霉素48小时以上。我们在治疗期间收集了有关万古霉素剂量和血药浓度的数据。急性肾损伤(AKI)定义为在万古霉素治疗期间或停药后72小时内,每日尿量<0.5 ml / kg / h和/或血清肌酐从基线水平增加≥0.3 mg / dl。进行多变量logistic回归分析以识别AKI的预测因子。结果:在符合入选标准的207位患者中,有50位(24%)发展为AKI。这些患者病情较重,入院时肌酐清除率较低,在治疗的前三天(C均值)更常接触其他肾毒性药物,治疗时间更长,万古霉素浓度更高(C均值)。 C均值与早期AKI(距治疗开始后48小时内)以及万古霉素给药持续时间与晚期AKI独立相关。结论:在连续输注万古霉素治疗的危重患者中,近25%发生AKI。万古霉素浓度和治疗持续时间分别是与治疗期间早期和晚期AKI发生有关的最强变量。

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