Shoulders Bethany R, Crow Jessica R, Davis Stephanie L, Whitman Glenn J, Gavin Melanie, Lester Laeban, Barodka Viachaslau, Dzintars Kathryn
Department of Pharmacy, The Johns Hopkins Hospital, Baltimore, Maryland.
Anesthesiology and Critical Care Medicine, The Johns Hopkins Hospital, Baltimore, Maryland.
Pharmacotherapy. 2016 Feb;36(2):166-73. doi: 10.1002/phar.1689. Epub 2016 Jan 22.
To determine whether intraoperative continuous-infusion (CI) cefazolin reduces the incidence of surgical site infections (SSIs) compared with intermittent (INT) cefazolin dosing in patients undergoing coronary artery bypass grafting (CABG) on cardiopulmonary bypass (CPB); safety end points and protocol adherence comparing the two dosing strategies were also explored.
Retrospective quasi-experimental (pre-post intervention) cohort study.
Large academic medical center.
A total of 516 adults who underwent CABG on CPB and received cefazolin intraoperatively between June 1, 2013, and December 31, 2014, were included. The INT cohort included 284 patients who underwent CABG from June 2013 to February 2014. The CI cohort included 232 patients who underwent CABG from April to December 2014, after an intraoperative CI cefazolin protocol for cardiac surgery patients undergoing CPB was adopted in March 2014.
The primary end point was incidence of SSIs, and safety end points of renal dysfunction and seizures were evaluated. Multivariable logistic regression analysis was used to determine the impact on SSIs when controlling for other risk factors. A subgroup analysis for this study included 2 months within each time period to evaluate protocol adherence. The overall incidence of SSIs was decreased in patients receiving CI cefazolin, although this did not reach statistical significance (4.6% in the INT cohort vs 1.7% in the CI cohort, p=0.116). Superficial SSIs were significantly reduced in the CI cohort (2.8% in the INT cohort vs 0.4% in the CI cohort, p=0.039). In the regression analysis, CI cefazolin decreased the odds of SSI by 66%, although it did not reach statistical significance (p=0.077). Safety end points were not significantly different between groups. Overall protocol adherence did not differ significantly between the cohorts: 77% in the INT cohort and 67% in the CI cohort (p=0.212).
CI cefazolin significantly decreased the incidence of superficial SSIs compared with INT cefazolin in patients undergoing CABG on CPB, without increasing the risk for adverse effects. As this study was underpowered to detect a significant difference in overall SSIs, larger, randomized studies are required to validate the superiority of CI cefazolin.
确定在接受体外循环(CPB)冠状动脉搭桥术(CABG)的患者中,术中持续输注(CI)头孢唑林与间歇性(INT)给药相比,是否能降低手术部位感染(SSI)的发生率;还探讨了比较两种给药策略的安全性终点和方案依从性。
回顾性准实验(干预前后)队列研究。
大型学术医疗中心。
纳入了2013年6月1日至2014年12月31日期间在CPB下行CABG并在术中接受头孢唑林治疗的516名成年人。INT队列包括2013年6月至2014年2月接受CABG的284名患者。CI队列包括2014年4月至12月接受CABG的232名患者,此前于2014年3月采用了针对接受CPB的心脏手术患者的术中CI头孢唑林方案。
主要终点为SSI的发生率,并评估肾功能不全和癫痫发作的安全性终点。采用多变量逻辑回归分析来确定在控制其他危险因素时对SSI的影响。本研究的亚组分析包括每个时间段内的2个月,以评估方案依从性。接受CI头孢唑林的患者中SSI的总体发生率有所降低,尽管未达到统计学意义(INT队列中为4.6%,CI队列中为1.7%,p=0.116)。CI队列中浅表SSI显著减少(INT队列中为2.8%,CI队列中为0.4%,p=0.039)。在回归分析中,CI头孢唑林使SSI的几率降低了66%,尽管未达到统计学意义(p=0.077)。两组之间的安全性终点无显著差异。队列之间的总体方案依从性无显著差异:INT队列中为77%,CI队列中为67%(p=0.212)。
与INT头孢唑林相比,CI头孢唑林在接受CPB的CABG患者中显著降低了浅表SSI的发生率,且未增加不良反应风险。由于本研究检测总体SSI显著差异的能力不足,因此需要更大规模的随机研究来验证CI头孢唑林的优越性。
