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Clinical Trial
. 2019 Oct;75(10):1393-1404.
doi: 10.1007/s00228-019-02708-y. Epub 2019 Jul 16.

Dose rationale and pharmacokinetics of dexmedetomidine in mechanically ventilated new-borns: impact of design optimisation

Sven C van Dijkman  1 Pieter A J G De Cock  2   3 Koenraad Smets  4 Wim Decaluwe  5 Anne Smits  6 Karel Allegaert  7   8 Johan Vande Walle  9 Peter De Paepe  2 Oscar Della Pasqua  10   11
Affiliations
Clinical Trial

Dose rationale and pharmacokinetics of dexmedetomidine in mechanically ventilated new-borns: impact of design optimisation

Sven C van Dijkman et al. Eur J Clin Pharmacol. 2019 Oct.

Abstract

Purpose: There is a need for alternative analgosedatives such as dexmedetomidine in neonates. Given the ethical and practical difficulties, protocol design for clinical trials in neonates should be carefully considered before implementation. Our objective was to identify a protocol design suitable for subsequent evaluation of the dosing requirements for dexmedetomidine in mechanically ventilated neonates.

Methods: A published paediatric pharmacokinetic model was used to derive the dosing regimen for dexmedetomidine in a first-in-neonate study. Optimality criteria were applied to optimise the blood sampling schedule. The impact of sampling schedule optimisation on model parameter estimation was assessed by simulation and re-estimation procedures for different simulation scenarios. The optimised schedule was then implemented in a neonatal pilot study.

Results: Parameter estimates were more precise and similarly accurate in the optimised scenarios, as compared to empirical sampling (normalised root mean square error: 1673.1% vs. 13,229.4% and relative error: 46.4% vs. 9.1%). Most importantly, protocol deviations from the optimal design still allowed reasonable parameter estimation. Data analysis from the pilot group (n = 6) confirmed the adequacy of the optimised trial protocol. Dexmedetomidine pharmacokinetics in term neonates was scaled using allometry and maturation, but results showed a 20% higher clearance in this population compared to initial estimates obtained by extrapolation from a slightly older paediatric population. Clearance for a typical neonate, with a post-menstrual age (PMA) of 40 weeks and weight 3.4 kg, was 2.92 L/h. Extension of the study with 11 additional subjects showed a further increased clearance in pre-term subjects with lower PMA.

Conclusions: The use of optimal design in conjunction with simulation scenarios improved the accuracy and precision of the estimates of the parameters of interest, taking into account protocol deviations, which are often unavoidable in this event-prone population.

Keywords: Clinical trial simulations; Dexmedetomidine; Dose rationale; Extrapolation; Optimal design; Paediatrics; Pharmacokinetic modelling; Sparse sampling.

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References

    1. Brain Res Mol Brain Res. 1992 Nov;16(1-2):57-63 - PubMed
    1. BMC Pediatr. 2003 Dec 16;3:13 - PubMed
    1. Comput Methods Programs Biomed. 2004 Apr;74(1):29-46 - PubMed
    1. Proc (Bayl Univ Med Cent). 2001 Jan;14(1):13-21 - PubMed
    1. JAMA. 2007 Dec 12;298(22):2644-53 - PubMed

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