Population Pharmacokinetic Analysis of Ibuprofen Enantiomers in Preterm Newborn Infants

Grégoire, Nicolas; Desfrère, Luc; Rozé, Jean‐Christophe; Kibleur, Yves; Koehne, Petra

doi:10.1177/0091270008323752

Cited by 24 publications

(40 citation statements)

References 24 publications

(38 reference statements)

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“…In addition, all post-immunization measurements were conducted at 18 hours, which potentially does not represent a similar time point in the inflammation kinetics of all patients. Further, because of the large inter individual variability in pharmacokinetics parameters of the active S (+)-ibuprofen enantiomere expected in this population of preterm infants 30 , we cannot exclude the possibility that the drug concentrations were not sufficient to significantly reduce PgE2 levels in a proportion of infants, while sufficient to mitigate the CRE elevation response to immunization. We are not aware of other studies reporting measures of PgE2 after immunization in infants.…”

Section: Discussionmentioning

confidence: 98%

Cardio-respiratory Events and Inflammatory Response After Primary Immunization in Preterm Infants < 32 Weeks Gestational Age: A Randomized Controlled Study

Jmaa

Hernández

Sutherland

et al. 2017

Pediatric Infectious Disease Journal

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The first immunization of infants born < 32 weeks was associated with an increase in CRP. Ibuprofen treatment significantly attenuated the variation (Δ) in CRE following first immunization in these infants but the current study could not demonstrate an impact on CRP and PgE2 levels. The impact of anti-inflammatory treatment on antigenicity must be evaluated before their clinical use aiming at reducing CRE after immunization in preterm infants.

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Section: Discussionmentioning

confidence: 98%

Cardio-respiratory Events and Inflammatory Response After Primary Immunization in Preterm Infants < 32 Weeks Gestational Age: A Randomized Controlled Study

Jmaa

Hernández

Sutherland

et al. 2017

Pediatric Infectious Disease Journal

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“…Similarly, adaptations in either the route of administration (oral versus intravenous) or the use of enantiomer specific solutions have to be evaluated on their potential benefits compared to the currently implemented dosing regimes [36,37]. Others reported on the improved renal tolerance to indomethacin when continuous administration was compared to intermittent ‘bolus’ administration [38].…”

Section: General Discussion and Conclusionmentioning

confidence: 99%

Renal Side Effects of Non-Steroidal Anti-Inflammatory Drugs in Neonates

et al. 2010

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Non-steroidal anti-inflammatory drugs like ibuprofen or indomethacin are commonly prescribed drugs to induce pharmacologic closure of a patent ductus arteriosus in preterm neonates. Based on a recently published Cochrane meta-analysis, both drugs are equally effective to induce closure. Drug choice can therefore be based on differences in side effects or pharmaco-economic arguments. The current review quantifies the negative impact of either ibuprofen or indomethacin on renal function, including diuresis, glomerular filtration rate and renal tubular function. Both ibuprofen and indomethacin have a quantifiable impact on renal function. However, compared to ibuprofen, the negative impact of indomethacin is more pronounced.

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“…The population PK models (see Supplementary File 1) were compared with respect to birth weight, gestational age (GA), and postnatal age (PNA) of the cohort, ibuprofen-dosing regimen, route of administration, and studied ibuprofen enantiomers [12, 22, 23, 30, 31]. …”

Section: Methodsmentioning

confidence: 99%

Simulation-based suggestions to improve ibuprofen dosing for patent ductus arteriosus in preterm newborns

Flint

Heine

Spaans

et al. 2018

Eur J Clin Pharmacol

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PurposeIbuprofen is the drug of choice for treatment of patent ductus arteriosus (PDA). There is accumulating evidence that current ibuprofen-dosing regimens for PDA treatment are inadequate. We aimed to propose an improved dosing regimen, based on all current knowledge.MethodsWe performed a literature search on the clinical pharmacology and effectiveness of ibuprofen. (R)- and (S)-ibuprofen plasma concentration-time profiles of different dosing regimens were simulated using a population pharmacokinetic model and evaluated to obtain a safe, yet likely more efficacious ibuprofen exposure.ResultsThe most effective intravenous ibuprofen dosing in previous clinical trials included a first dose of 20 mg kg−1 followed by 10 mg kg−1 every 24 h. Simulations of this dosing regimen show an (S)-ibuprofen trough concentration of 43 mg L−1 is reached at 48 h, which we assumed the target through concentration. We show that this target can be reached with a first dose of 18 mg kg−1, followed by 4 mg kg−1 every 12 h. After 96 h postnatal age, the dose should be increased to 5 mg kg−1 every 12 h due to maturation of clearance. This twice-daily dosing has the advantage over once-daily dosing that an effective trough level may be maintained, while peak concentrations are substantially (22%) lower.ConclusionsWe propose to improve intermittent ibuprofen-dosing regimens by starting with a high first dose followed by a twice-daily maintenance dosing regimen that requires increase over time and should be continued until sufficient effect has been achieved.Electronic supplementary materialThe online version of this article (10.1007/s00228-018-2529-y) contains supplementary material, which is available to authorized users.

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Population Pharmacokinetic Analysis of Ibuprofen Enantiomers in Preterm Newborn Infants

Cited by 24 publications

References 24 publications

Cardio-respiratory Events and Inflammatory Response After Primary Immunization in Preterm Infants < 32 Weeks Gestational Age: A Randomized Controlled Study

Cardio-respiratory Events and Inflammatory Response After Primary Immunization in Preterm Infants < 32 Weeks Gestational Age: A Randomized Controlled Study

Renal Side Effects of Non-Steroidal Anti-Inflammatory Drugs in Neonates

Simulation-based suggestions to improve ibuprofen dosing for patent ductus arteriosus in preterm newborns

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