Oral Ibuprofen Is More Effective than Intravenous Ibuprofen for Closure of a Patent Ductus Arteriosus: Can Pharmacokinetic Modeling Help Us to Understand Why?

IF 2.6 3区 医学 Q1 PEDIATRICS Neonatology Pub Date : 2023-01-01 DOI:10.1159/000526210
Cornelis Smit, Aline G J Engbers, Samira Samiee-Zafarghandy, Tamara van Donge, Sinno H P Simons, Robert B Flint, Marc Pfister, Catherijne A J Knibbe, John N van den Anker
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引用次数: 2

Abstract

Introduction: Oral ibuprofen is more effective than intravenous (IV) ibuprofen for closure of a patent ductus arteriosus (PDA). This study explored whether higher concentrations of the biologically active S-enantiomer or increased R- to S-conversion following oral dosing could explain this finding.

Methods: Two datasets containing 370 S- and R-ibuprofen concentrations from 95 neonates with PDA treated with oral (n = 27, 28%) or IV ibuprofen were analyzed using nonlinear mixed effects modeling. Concentration-time profiles in typical neonates were explored and compared in different dosing or R- to S-conversion scenarios.

Results: Postnatal age (PNA), gestational age (GA), and being small for GA impacted S- and R-ibuprofen clearance. Upon oral dosing, S-ibuprofen concentrations were lower compared to IV ibuprofen for a large part of the dosing interval. We could show that R- to S-conversion will not exceed 45%. Exploration of a 30% presystemic R- to S-conversion resulted in a 25-32% increase in S-ibuprofen exposure following oral administration with AUC72h values varying between 700-2,213 mg*h/L (oral) and 531-1,762 (IV) for the standard or 1,704-2,893 (oral) and 1,295-2,271 mg*h/L (IV) for PNA-based dosing.

Discussion: The absence of higher S-ibuprofen concentrations does not support a beneficial concentration-time profile after oral dosing. While a fraction of up to 45% presystemic R- to S-conversion could not be ruled out, the impact of such a low conversion might be only relevant for the standard but not high dosing regimens, considering reported exposure-response targets. Perhaps, the lack of high peak concentrations observed following IV dosing may play a role in the observed effects upon oral dosing.

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口服布洛芬对动脉导管未闭闭合比静脉注射布洛芬更有效:药代动力学模型能帮助我们理解原因吗?
简介:对于动脉导管未闭(PDA)的闭合,口服布洛芬比静脉注射(IV)布洛芬更有效。本研究探讨了是否较高的生物活性s -对映体浓度或口服给药后R-到s -转化的增加可以解释这一发现。方法:采用非线性混合效应模型分析95例口服(n = 27,28%)或静脉注射布洛芬的PDA新生儿370 S-和r -布洛芬浓度。在不同剂量或R- s转换情景下,对典型新生儿的浓度-时间分布进行了探讨和比较。结果:出生年龄(PNA)、胎龄(GA)和胎龄小影响S-和r -布洛芬清除率。口服给药后,s -布洛芬浓度在给药间隔的大部分时间内低于静脉给药。我们可以证明R-到s -的转换不会超过45%。探索30%的系统前R-到s -转化导致口服给药后s -布洛芬暴露增加25-32%,AUC72h值在700- 2213 mg*h/L(口服)和531- 1762 (IV)之间变化,或在pna -基给药的1704 - 2893(口服)和1295 - 2271 mg*h/L (IV)之间变化。讨论:没有较高的s -布洛芬浓度并不支持口服给药后有益的浓度-时间分布。虽然不能排除高达45%的系统前R-到s转换的一小部分,但考虑到报告的暴露反应目标,这种低转换的影响可能只与标准而非高剂量方案有关。也许,静脉给药后观察到的缺乏高峰浓度可能在口服给药后观察到的效应中起作用。
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来源期刊
Neonatology
Neonatology 医学-小儿科
CiteScore
0.60
自引率
4.00%
发文量
91
审稿时长
6-12 weeks
期刊介绍: This highly respected and frequently cited journal is a prime source of information in the area of fetal and neonatal research. Original papers present research on all aspects of neonatology, fetal medicine and developmental biology. These papers encompass both basic science and clinical research including randomized trials, observational studies and epidemiology. Basic science research covers molecular biology, molecular genetics, physiology, biochemistry and pharmacology in fetal and neonatal life. In addition to the classic features the journal accepts papers for the sections Research Briefings and Sources of Neonatal Medicine (historical pieces). Papers reporting results of animal studies should be based upon hypotheses that relate to developmental processes or disorders in the human fetus or neonate.
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