新生儿重症监护室中有晚期败血症风险的住院婴儿停用抗生素后的暴露情况。

IF 2.9 4区 医学 Q3 IMMUNOLOGY Pediatric Infectious Disease Journal Pub Date : 2024-10-01 Epub Date: 2024-06-17 DOI:10.1097/INF.0000000000004426
Kelly C Wade, Rachel G Greenberg, Daniel K Benjamin, Lydia Li-Hui Chen, Brandon Vo, Berwyn Liselle Ang, Angelique Boutzoukas, Kanecia Zimmerman, Reese H Clark, Michael Cohen-Wolkowiez, Jennifer Le
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Monte Carlo simulations (NONMEM 7.3) were used to predict steady-state exposures after a 72-hour antibiotic course per Neofax dosing. Exposure was assessed relative to drug-specific minimum inhibitory concentration (MIC) targets between 1 and 16 mcg/mL for Pseudomonas and Enterobacteriaceae species. Postdiscontinuation antibiotic exposure (PDAE) was defined as the time from the last dose to when antibiotic concentration decreased below a specific MIC.</p><p><strong>Results: </strong>Piperacillin-tazobactam, cefepime and tobramycin cohorts included infants with median gestation age 29, 32 and 32 weeks and postnatal age 17, 19 and 15 days, respectively. The mean PDAE was 19-68 hours, depending on the specific antibiotic/MIC combination. PDAE was longer for infants <28 days old and preterm (vs. term) infants. Cefepime exhibited the longest mean PDAE of 68 hours for Enterobacteriaceae MIC 1. Piperacillin mean PDAE was 25 hours for Enterobacteriaceae MIC 8. 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引用次数: 0

摘要

背景:在新生儿重症监护室,婴儿有晚期败血症的风险。当血液培养呈阴性时,抗生素监管工作鼓励停止使用抗生素,但最后一次用药后的治疗暴露持续时间尚不清楚:这项模拟抗生素暴露的回顾性队列研究使用了已发表的群体药代动力学模型,该模型针对早产儿和足月儿、出生后 7-60 天、暴露于头孢吡肟、哌拉西林-他唑巴坦或妥布霉素的新生儿重症监护室特定药物队列。蒙特卡洛模拟(NONMEM 7.3)用于预测按新法给药 72 小时抗生素疗程后的稳态暴露量。针对假单胞菌和肠杆菌科菌种,根据药物特异性最低抑菌浓度 (MIC) 目标值(1 至 16 微克/毫升)评估暴露量。停药后抗生素暴露(PDAE)定义为从最后一次用药到抗生素浓度降至特定 MIC 以下的时间:哌拉西林-他唑巴坦、头孢吡肟和妥布霉素队列中的婴儿妊娠中位年龄分别为 29 周、32 周和 32 周,产后年龄分别为 17 天、19 天和 15 天。平均 PDAE 为 19-68 小时,取决于特定的抗生素/MIC 组合。婴儿的 PDAE 更长 结论哌拉西林和头孢吡肟的暴露在预期的 8 至 12 小时用药间隔后很长时间内仍具有治疗作用。对于住院婴儿,尤其是早产儿和出生后 1 个月内的婴儿,PDAE 是抗生素管理的一个重要考虑因素。
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Postdiscontinuation Antibiotic Exposure in Hospitalized Infants at Risk for Late-onset Sepsis in the Neonatal Intensive Care Unit.

Background: In the neonatal intensive care unit, infants are at risk for late-onset sepsis. When blood cultures are negative, antibiotic stewardship efforts encourage stopping antibiotics, yet the duration of therapeutic exposure after the last dose is unknown.

Methods: This retrospective cohort study of simulated antibiotic exposures used published population pharmacokinetic models within drug-specific neonatal intensive care unit cohorts of preterm and term infants, postnatal age 7-60 days and exposed to cefepime, piperacillin-tazobactam or tobramycin. Monte Carlo simulations (NONMEM 7.3) were used to predict steady-state exposures after a 72-hour antibiotic course per Neofax dosing. Exposure was assessed relative to drug-specific minimum inhibitory concentration (MIC) targets between 1 and 16 mcg/mL for Pseudomonas and Enterobacteriaceae species. Postdiscontinuation antibiotic exposure (PDAE) was defined as the time from the last dose to when antibiotic concentration decreased below a specific MIC.

Results: Piperacillin-tazobactam, cefepime and tobramycin cohorts included infants with median gestation age 29, 32 and 32 weeks and postnatal age 17, 19 and 15 days, respectively. The mean PDAE was 19-68 hours, depending on the specific antibiotic/MIC combination. PDAE was longer for infants <28 days old and preterm (vs. term) infants. Cefepime exhibited the longest mean PDAE of 68 hours for Enterobacteriaceae MIC 1. Piperacillin mean PDAE was 25 hours for Enterobacteriaceae MIC 8. Tobramycin had a short mean PDAE of 19 hours.

Conclusions: Piperacillin and cefepime exposures remained therapeutic long after the expected 8- to 12-hour dosing interval. PDAE is an important consideration for antibiotic stewardship among hospitalized infants, particularly premature infants and those within 1 month postbirth.

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来源期刊
CiteScore
6.30
自引率
2.80%
发文量
566
审稿时长
2-4 weeks
期刊介绍: ​​The Pediatric Infectious Disease Journal® (PIDJ) is a complete, up-to-the-minute resource on infectious diseases in children. Through a mix of original studies, informative review articles, and unique case reports, PIDJ delivers the latest insights on combating disease in children — from state-of-the-art diagnostic techniques to the most effective drug therapies and other treatment protocols. It is a resource that can improve patient care and stimulate your personal research.
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