Morphine pharmacokinetics and pharmacodynamics in preterm and term neonates: secondary results from the NEOPAIN trial

doi:10.1093/bja/aen248

BJA Advance Access originally published online on August 23, 2008
British Journal of Anaesthesia 2008 101(5):680-689; doi:10.1093/bja/aen248

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Morphine pharmacokinetics and pharmacodynamics in preterm and term neonates: secondary results from the NEOPAIN trial

K. J. S. Anand¹^,*, B. J. Anderson², N. H. G. Holford³, R. W. Hall¹, T. Young⁴, B. Shephard⁵, N. S. Desai⁶, B. A. Barton⁷ for the NEOPAIN Trial Investigators Group

¹ Department of Pediatrics, University of Arkansas for Medical Sciences, Little Rock, AR, USA
² Division of Anaesthesiology
³ Division of Pharmacology and Clinical Pharmacology, School of Medicine, University of Auckland, New Zealand
⁴ University of North Carolina at Chapel Hill and Wake Medical Center, Raleigh, NC, USA
⁵ Tufts University School of Medicine, Boston, MA, USA
⁶ University of Kentucky Medical Center, Lexington, KY, USA
⁷ Maryland Medical Research Institute, Baltimore, MD, USA

^* Corresponding author: Arkansas Children's Hospital, Rm S-4417, 800 Marshall Street, Slot 900, Little Rock, AR 72202, USA. E-mail: anandsunny{at}uams.edu

Background: Relationships between plasma morphine concentrations and neonatalresponses to endotracheal tube (ETT) suctioning are unknownin preterm neonates.

Methods: Ventilated preterm neonates (n=898) from 16 centres were randomlyassigned to placebo (n=449) or morphine (n=449). After an i.v.loading dose (100 µg kg^–1), morphine infusions [23–26weeks postmenstrual age (PMA) 10 µg kg^–1 h^–1;27–29 weeks 20 µg kg^–1 h^–1; and 30–32weeks 30 µg kg^–1 h^–1] were established fora maximum of 14 days. Open-label morphine (20–100 µgkg^–1) was given for pain or agitation. Morphine assayand neonatal response to ETT suctioning was measured at 20–28and 70–76 h after starting the drug infusion and at 10–14h after discontinuation of the study drug. The concentration–effectresponse was investigated using non-linear mixed effects models.

Results: A total of 5119 data points (1598 measured morphine concentrationsand 3521 effect measures) were available from 875 neonates foranalysis. Clearance was 50% that of the mature value at 54.2weeks PMA (CLmat₅₀) and increased from 2.05 litre h^–170 kg^–1 at 24 weeks PMA to 6.04 litre h^–1 70 kg^–1at 32 weeks PMA. The volume of distribution in preterm neonateswas 190 litre 70 kg^–1 (CV 51%) and did not change withage. There was no relationship between morphine concentrations(range 0–440 µg litre^–1) and heart rate changesassociated with ETT suctioning or with the Premature InfantPain Profile.

Conclusions: A sigmoid curve describing maturation of morphine clearanceis moved to the right in preterm neonates and volume of distributionis increased compared with term neonates. Morphine does notalter the neonatal response to ETT suctioning.

Keywords: anaesthesia, paediatric; anaesthetic–analgesic regimens; analgesics opioid, morphine; model, pharmacodynamic; model, pharmacokinetic

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