持续肾脏替代治疗的危重症患者中治疗药物监测指导下的哌拉西林给药:一项系统评价
Therapeutic drug monitoring-guided piperacillin dosing in critically ill patients undergoing continuous renal replacement therapy: a systematic review.
作者信息
Mohd Rozi Nazatul Adhwa, Mohd Tahir Nor Asyikin, Mohd Saffian Shamin, Makmor-Bakry Mohd, Mohamad Yusof Aliza, Mustafar Ruslinda, M Saud Muhammad Nordin
机构信息
Centre for Quality Management of Medicines, Faculty of Pharmacy, Universiti Kebangsaan Malaysia, Jalan Raja Muda Aziz, 50300 Kuala Lumpur, Malaysia.
Faculty of Pharmacy, Universitas Airlangga, PQMM+9Q6, Gedung Nanizar Zaman Joenoes Kampus C UNAIR, Jl. Mulyorejo, Mulyorejo, Surabaya, East Java 60115, Indonesia.
出版信息
J Antimicrob Chemother. 2024 Dec 2;79(12):3078-3090. doi: 10.1093/jac/dkae332.
BACKGROUND
Continuous renal replacement therapy (CRRT) complicates antibiotic dosing in critically ill patients due to altered pharmacokinetics. The optimal dosing of piperacillin remains unclear. Therapeutic drug monitoring (TDM) can personalize piperacillin therapy and improve outcomes.
OBJECTIVES
This review investigates the effects of TDM-guided piperacillin dosing on pharmacokinetic target attainment and clinical outcomes in CRRT patients, analyses correlations with clinical outcomes, provides optimal dosing strategies for piperacillin and identifies future research areas.
METHODS
A systematic search of PubMed, Scopus and Web of Science was conducted until December 2023, identifying studies on piperacillin pharmacokinetics and clinical outcomes in adult CRRT patients. Data on study characteristics, piperacillin exposures, TDM use, target attainment rates, mortality and length of stay were extracted. The risk of bias was assessed using the Newcastle-Ottawa Scale.
RESULTS
Eleven observational studies were included. High pharmacokinetic variability was evident, with piperacillin target non-attainment in up to 74% of cases without TDM. Two studies with routine TDM showed increased target attainment rates of 80%-100%. Mortality ranged from 17% to 56%, with supratherapeutic concentrations (≥100 mg/L) associated with higher mortality. The impact of optimized piperacillin exposures on outcomes was inconclusive. Most studies demonstrated a low risk of bias.
CONCLUSIONS
TDM-guided piperacillin dosing in CRRT patients improved target attainment rates (≥80%). Mortality rates ranged from 17% to 56%, with inconsistent correlations between drug exposures and survival. Supratherapeutic concentrations were linked to higher mortality. Standardized TDM protocols are needed. Future research should establish clear exposure-response relationships and the impact of TDM on clinical outcomes.
背景
由于药代动力学改变,持续肾脏替代治疗(CRRT)使重症患者的抗生素给药变得复杂。哌拉西林的最佳给药剂量仍不明确。治疗药物监测(TDM)可使哌拉西林治疗个体化并改善治疗效果。
目的
本综述研究TDM指导下的哌拉西林给药对CRRT患者药代动力学目标达成情况及临床结局的影响,分析与临床结局的相关性,提供哌拉西林的最佳给药策略,并确定未来的研究领域。
方法
对PubMed、Scopus和Web of Science进行系统检索,直至2023年12月,以确定关于成年CRRT患者哌拉西林药代动力学和临床结局的研究。提取有关研究特征、哌拉西林暴露情况、TDM使用情况、目标达成率、死亡率和住院时间的数据。使用纽卡斯尔-渥太华量表评估偏倚风险。
结果
纳入了11项观察性研究。药代动力学变异性很高,在无TDM的情况下,高达74%的病例未达到哌拉西林目标值。两项采用常规TDM的研究显示目标达成率提高至80%-100%。死亡率在17%至56%之间,治疗浓度高于治疗浓度(≥100 mg/L)与较高死亡率相关。优化的哌拉西林暴露对结局的影响尚无定论。大多数研究显示偏倚风险较低。
结论
TDM指导下的CRRT患者哌拉西林给药提高了目标达成率(≥80%)。死亡率在17%至56%之间,药物暴露与生存之间的相关性不一致。治疗浓度高于治疗浓度与较高死亡率相关。需要标准化的TDM方案。未来的研究应建立明确的暴露-反应关系以及TDM对临床结局的影响。
Zotero 插件