Rady Faculty of Health Sciences, University of Manitoba, 750 McDermot Avenue, Winnipeg, Manitoba, R3E 0T5, Canada.
St Boniface Hospital, 409 Taché Avenue, Winnipeg, Manitoba, R2H 2A6, Canada.
J Antimicrob Chemother. 2018 Mar 1;73(3):768-771. doi: 10.1093/jac/dkx439.
Although clinical practice guidelines recommend standard cefazolin antimicrobial prophylaxis (AP) dosing for cardiac surgery, limited data exist as to whether adequate concentrations are achieved in this patient population. The goal of our study was to characterize intraoperative cefazolin concentrations particularly at wound closure with regards to maintaining target cefazolin closure concentrations ≥40 mg/L.
Adults undergoing cardiac surgery with cardiopulmonary bypass (CPB) and receiving cefazolin AP according to protocol were studied. Blood samples were collected after the preoperative cefazolin dose, prior to intraoperative cefazolin doses and at wound closure. Intraoperative trough and closure concentrations were characterized and evaluated against a target threshold of ≥ 40 mg/L (≥8 mg/L unbound, assuming 80% protein binding).
Fifty-five subjects (64.9 ± 10.4 years, 89.7 ± 16.5 kg, CLCR >50 mL/min/72 kg) completed the study. Total cefazolin concentrations were <40 mg/L in 40% (12 of 30) of intraoperative trough samples and 9.8% (5 of 51) of closure samples. Below-target concentrations at some time during surgery were documented in 30.9% (17 of 55) of subjects. In multivariate analyses, lower body weight (P = 0.027) and shorter duration of surgery (P = 0.045) were significant predictors of closure concentrations <40 mg/L. A total cefazolin exposure (preoperative and intraoperative doses) of ≥ 7.6 mg/kgdosing weight for every hour of surgery (intermittent dosing) was required to achieve target closure concentrations.
The standard cefazolin AP regimen was not reliable in maintaining target closure concentrations ≥40 mg/L in patients with normal renal function undergoing elective cardiac surgery with CPB. The findings supported a cefazolin AP regimen consisting of at least 2 g preoperatively and every 3 h during surgery.
尽管临床实践指南推荐心脏手术采用标准头孢唑林抗菌预防(AP)剂量,但关于该人群中是否能达到足够的浓度,相关数据有限。本研究的目的是研究术中头孢唑林浓度,特别是在切口关闭时,以维持目标头孢唑林关闭浓度≥40mg/L。
研究了接受体外循环(CPB)心脏手术并根据方案接受头孢唑林 AP 的成年人。在术前头孢唑林剂量后、术中头孢唑林剂量前和切口关闭时采集血样。描述了术中谷浓度和关闭浓度,并针对≥40mg/L(假设 80%蛋白结合,无结合物≥8mg/L)的目标阈值进行了评估。
55 名受试者(64.9±10.4 岁,89.7±16.5kg,CLCR>50mL/min/72kg)完成了研究。术中谷浓度样本中,40%(30 个样本中的 12 个)和关闭样本中 9.8%(51 个样本中的 5 个)的总头孢唑林浓度<40mg/L。术中某个时间点记录到低于目标浓度的情况在 30.9%(55 名受试者中的 17 名)中。在多变量分析中,较低的体重(P=0.027)和较短的手术持续时间(P=0.045)是关闭浓度<40mg/L 的显著预测因素。对于每小时手术(间歇性给药),头孢唑林总暴露量(术前和术中剂量)需要≥7.6mg/kg 给药体重才能达到目标关闭浓度。
对于接受 CPB 心脏手术的肾功能正常的择期患者,标准头孢唑林 AP 方案不能可靠地维持目标关闭浓度≥40mg/L。研究结果支持使用至少术前 2g 和手术期间每 3 小时一次的头孢唑林 AP 方案。
