Pharmacogenetics of codeine metabolism in an urban population of children and its implications for analgesic reliability

doi:10.1093/bja/aef284

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British Journal of Anaesthesia, 2002, Vol. 89, No. 6 839-845
© 2002 The Board of Management and Trustees of the British Journal of Anaesthesia

Clinical Investigations

Pharmacogenetics of codeine metabolism in an urban population of children and its implications for analgesic reliability

D. G. Williams¹^,2, A. Patel³ and R. F. Howard^*^,4

¹ Anaesthetic Department, The Royal London Hospital, Whitechapel, London E1 1BB, UK. ² Portex Department of Anaesthesia, Institute of Child Health, Guilford Street, London WC1N 1EH, UK. ³ Anaesthetic Department, The Royal National Throat, Nose and Ear Hospital, Grays Inn Road, London WC1X 8DA, UK. ⁴ Department of Anaesthesia, Great Ormond Street Hospital for Children NHS Trust and Children Nationwide Pain Research Centre, Great Ormond Street, London WC1N 3JN, UK r.howard@ich.ucl.ac.uk

Background. Codeine analgesia is wholly or mostly due to itsmetabolism to morphine by the cytochrome P450 enzyme CYP2D6,which shows significant genetic variation in activity. The aimsof this study were to investigate genotype, phenotype and morphineproduction from codeine in children undergoing adenotonsillectomy,and to compare analgesia from codeine or morphine combined withdiclofenac.

Methods. Ninety-six children received either codeine 1.5 mg kg^–1or morphine 0.15 mg kg^–1 in a randomized, double-blinddesign. Genetic analysis was performed and plasma morphine concentrationsat 1 h were determined. Postoperative analgesia and side-effectswere recorded.

Results. Forty-seven per cent of children had genotypes associatedwith reduced enzyme activity. Mean (SD) morphine concentrationswere significantly lower (P<0.001) after codeine [4.5 (0.3)ng ml^–1] than after morphine [24.7 (1.5) ng ml^–1],and morphine and its metabolites were not detected in 36% ofchildren given codeine. There was a significant relationshipbetween phenotype and plasma morphine (P=0.02). More childrenrequired rescue analgesia after codeine at both 2 (P<0.05)and 4 h after administration (P<0.01). Fifty-six per centof children vomited after morphine and 29% after codeine (P<0.01).Neither phenotype nor morphine concentration was correlatedwith either pain score or the need for rescue analgesia (r=–0.21,95% confidence interval –0.4, –0.01).

Conclusions. Reduced ability for codeine metabolism may be morecommon than previously reported. Plasma morphine concentration1 h after codeine is very low, and related to phenotype.Codeine analgesia is less reliable than morphine, but was notwell correlated with either phenotype or plasma morphine inthis study.

Br J Anaesth 2002; 89: 839–45

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