Drake University College of Pharmacy and Health Sciences, Des Moines, Iowa.
Department of Clinical Pharmacy, University of Colorado Skaggs School of Pharmacy and Pharmaceutical Sciences, Aurora, Colorado.
Pharmacotherapy. 2018 Sep;38(9):921-934. doi: 10.1002/phar.2156. Epub 2018 Jul 20.
Neurocritically ill patients have clinically significant alterations in pharmacokinetic parameters of renally eliminated medications that may result in subtherapeutic plasma and cerebrospinal fluid antibiotic concentrations.
We conducted a prospective randomized open-label study of adult neurocritically ill patients treated with vancomycin and cefepime. Vancomycin 15 mg/kg and cefepime 2 g were dosed at every-8- or 12-hour intervals. The primary outcomes were the achievement of pharmacodynamic (PD) targets related to time of unbound drug above minimum inhibitory concentrations (MIC) for 60% or more of the dosing interval (fT > MIC ≥ 60%) for β-lactams and ratio of 24-hour area under the curve (AUC):MIC of 400 or greater for vancomycin.
Twenty patients were included in the study. They were divided equally between the every-12-hour and every-8-hour dosing groups. Patients (mean age 51.8 ± 11 yrs) were primarily male (60%) and white (95%), and most had an admission diagnosis of intracranial hemorrhage (80%). Compared with the every-12-hour group, the every-8-hour vancomycin group achieved target trough concentrations (higher than 15 μg/ml) significantly more frequently at initial measurement (0% vs 80%, p<0.01) and at 7-10 days (0% vs 90%, p=0.045) and achieved PD targets more frequently at increasing MICs. Similarly, compared with every-12-hour dosing, the every-8-hour cefepime dosing strategy significantly increased PD target attainment (fT > MIC ≥ 60%) at an MIC of 8 μg/ml (20% vs 70%, p=0.02).
This study demonstrated that more frequent dosing of vancomycin and cefepime is required to achieve optimal PD targets in adult neurocritically ill patients. The need for increased total daily doses is potentially secondary to the development of augmented renal clearance.
神经危重症患者的肾清除药物药代动力学参数发生显著变化,可能导致治疗窗内血药浓度和脑脊液药物浓度低于治疗水平。
我们对接受万古霉素和头孢吡肟治疗的成年神经危重症患者进行了一项前瞻性随机开放标签研究。万古霉素剂量为 15mg/kg,每 8 或 12 小时 1 次;头孢吡肟剂量为 2g,每 8 或 12 小时 1 次。主要结局是达到药效学(PD)目标,包括β-内酰胺类药物游离药物超过最低抑菌浓度(MIC)时间的 60%或以上(fT>MIC≥60%)和万古霉素 24 小时 AUC:MIC 比值达到 400 或以上。
共有 20 例患者纳入研究,随机分为每 12 小时和每 8 小时 1 次剂量组,每组 10 例。患者(平均年龄 51.8±11 岁)主要为男性(60%)和白人(95%),大多数入院诊断为颅内出血(80%)。与每 12 小时组相比,每 8 小时 1 次万古霉素组在初始测量(0%比 80%,p<0.01)和第 7-10 天(0%比 90%,p=0.045)时更频繁地达到目标谷浓度(高于 15μg/ml),且在 MIC 升高时更频繁地达到 PD 目标。同样,与每 12 小时给药相比,每 8 小时 1 次头孢吡肟给药策略显著增加了 MIC 为 8μg/ml 时的 PD 目标达成率(fT>MIC≥60%)(20%比 70%,p=0.02)。
本研究表明,神经危重症成年患者需要更频繁地给予万古霉素和头孢吡肟,以达到最佳 PD 目标。需要增加每日总剂量可能是由于增强的肾清除率所致。
