阿莫西林和苄青霉素治疗早发型新生儿败血症的评估:一项药代动力学外部验证和模拟研究。
Evaluation of amoxicillin and benzylpenicillin therapy in early-onset neonatal sepsis: a pharmacometric external validation and simulation study.
作者信息
Zwart Tom C, Eleftheriou Dimitra, Jansen Sophie J, van der Beek Martha T, Moes Dirk Jan A R, Völler Swantje, Bekker Vincent
机构信息
Department of Clinical Pharmacy and Toxicology, Leiden University Medical Center, Leiden, The Netherlands.
Department of Clinical Pharmacy, Haga Teaching Hospital, The Hague, The Netherlands.
出版信息
J Antimicrob Chemother. 2025 Aug 1;80(8):2214-2225. doi: 10.1093/jac/dkaf191.
BACKGROUND AND OBJECTIVES
Early-onset sepsis (EOS) poses a significant morbidity and mortality risk in neonates, for which early diagnosis and adequate antibiotic therapy is crucial. Amoxicillin and benzylpenicillin combined with aminoglycosides are often prescribed empirically for neonatal EOS but optimal dosing regimens are lacking. To evaluate the pharmacokinetics (PK), PTA and toxicity of amoxicillin and benzylpenicillin in (pre)term neonates with EOS, and define optimal dosing regimens.
METHODS
One hundred forty-five neonates [gestational age (GA): 24-42 weeks] with EOS treated with intravenous amoxicillin or benzylpenicillin, dosed as per the Dutch Pediatric Formulary (DPF), were included. Amoxicillin and benzylpenicillin were quantified in left-over samples during the first 48 h of life. First, the performance of nine paediatric amoxicillin and benzylpenicillin population PK models was evaluated. Second, the most appropriate models were used for simulation-based PTA and toxicity analyses, evaluating eight international neonatal dosing regimens. Third, simulation-based dose optimization was conducted.
RESULTS
The Bijleveld (amoxicillin) and Padari (benzylpenicillin) models adequately described the obtained PK data (N = 252). For amoxicillin, all regimens showed >90% PTA up to 100%fT > MIC but displayed GA-dependent toxicity potential (concentrations >110 mg/L), the DPF regimen excepted. By contrast, all benzylpenicillin regimens showed suboptimal PTA, often accompanied with GA-dependent toxicity potential (concentrations >50 mg/L). Simulations indicated GA-based intermittent dosing or continuous infusion as options to further optimize benzylpenicillin therapy.
CONCLUSIONS
(Pre)term neonates with EOS can be adequately treated with amoxicillin dosed as per the DPF regimen. By contrast, further optimization is warranted for benzylpenicillin, for which GA-based intermittent dosing or continuous infusion pose potential alternatives.
背景与目的
早发型败血症(EOS)在新生儿中具有较高的发病和死亡风险,早期诊断及充分的抗生素治疗至关重要。阿莫西林和苄青霉素联合氨基糖苷类药物常被经验性用于新生儿EOS治疗,但缺乏最佳给药方案。本研究旨在评估阿莫西林和苄青霉素在患有EOS的(早产)新生儿中的药代动力学(PK)、达到治疗浓度的概率(PTA)及毒性,并确定最佳给药方案。
方法
纳入145例患有EOS的新生儿[胎龄(GA):24 - 42周],他们接受了静脉注射阿莫西林或苄青霉素治疗,给药剂量按照荷兰儿科处方集(DPF)。在出生后的前48小时内,对剩余样本中的阿莫西林和苄青霉素进行定量分析。首先,评估了9种儿科阿莫西林和苄青霉素群体PK模型的性能。其次,使用最合适的模型进行基于模拟的PTA和毒性分析,评估8种国际新生儿给药方案。第三,进行基于模拟的剂量优化。
结果
Bijleveld(阿莫西林)和Padari(苄青霉素)模型充分描述了所获得的PK数据(N = 252)。对于阿莫西林,所有方案在100%fT > MIC时PTA均>90%,但除DPF方案外均显示出与GA相关的潜在毒性(浓度>110mg/L)。相比之下,所有苄青霉素方案的PTA均不理想,且常伴有与GA相关的潜在毒性(浓度>50mg/L)。模拟结果表明,基于GA的间歇给药或持续输注是进一步优化苄青霉素治疗的选择。
结论
患有EOS的(早产)新生儿可按照DPF方案给予阿莫西林进行充分治疗。相比之下,苄青霉素需要进一步优化,基于GA的间歇给药或持续输注可能是潜在的替代方案。
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