Literature DB >> 27335380

Pharmacogenetics for Safe Codeine Use in Sickle Cell Disease.

Roseann S Gammal1, Kristine R Crews2, Cyrine E Haidar1, James M Hoffman1, Donald K Baker1, Patricia J Barker1, Jeremie H Estepp3, Deqing Pei4, Ulrich Broeckel5, Winfred Wang3, Mitchell J Weiss3, Mary V Relling1, Jane Hankins3.   

Abstract

After postoperative deaths in children who were prescribed codeine, several pediatric hospitals have removed it from their formularies. These deaths were attributed to atypical cytochrome P450 2D6 (CYP2D6) pharmacogenetics, which is also implicated in poor analgesic response. Because codeine is often prescribed to patients with sickle cell disease and is now the only Schedule III opioid analgesic in the United States, we implemented a precision medicine approach to safely maintain codeine as an option for pain control. Here we describe the implementation of pharmacogenetics-based codeine prescribing that accounts for CYP2D6 metabolizer status. Clinical decision support was implemented within the electronic health record to guide prescribing of codeine with the goal of preventing its use after tonsillectomy or adenoidectomy and in CYP2D6 ultra-rapid and poor metabolizer (high-risk) genotypes. As of June 2015, CYP2D6 genotype results had been reported for 2468 unique patients. Of the 830 patients with sickle cell disease, 621 (75%) had a CYP2D6 genotype result; 7.1% were ultra-rapid or possible ultra-rapid metabolizers, and 1.4% were poor metabolizers. Interruptive alerts recommended against codeine for patients with high-risk CYP2D6 status. None of the patients with an ultra-rapid or poor metabolizer genotype were prescribed codeine. Using genetics to tailor analgesic prescribing retained an important therapeutic option by limiting codeine use to patients who could safely receive and benefit from it. Our efforts represent an evidence-based, innovative medication safety strategy to prevent adverse drug events, which is a model for the use of pharmacogenetics to optimize drug therapy in specialized pediatric populations.
Copyright © 2016 by the American Academy of Pediatrics.

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Year:  2016        PMID: 27335380      PMCID: PMC4925073          DOI: 10.1542/peds.2015-3479

Source DB:  PubMed          Journal:  Pediatrics        ISSN: 0031-4005            Impact factor:   7.124


  49 in total

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3.  Codeine, ultrarapid-metabolism genotype, and postoperative death.

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7.  Randomized clinical trial of hydrocodone/acetaminophen versus codeine/acetaminophen in the treatment of acute extremity pain after emergency department discharge.

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Authors:  L J Rasmussen-Torvik; S C Stallings; A S Gordon; B Almoguera; M A Basford; S J Bielinski; A Brautbar; M H Brilliant; D S Carrell; J J Connolly; D R Crosslin; K F Doheny; C J Gallego; O Gottesman; D S Kim; K A Leppig; R Li; S Lin; S Manzi; A R Mejia; J A Pacheco; V Pan; J Pathak; C L Perry; J F Peterson; C A Prows; J Ralston; L V Rasmussen; M D Ritchie; S Sadhasivam; S A Scott; M Smith; A Vega; A A Vinks; S Volpi; W A Wolf; E Bottinger; R L Chisholm; C G Chute; J L Haines; J B Harley; B Keating; I A Holm; I J Kullo; G P Jarvik; E B Larson; T Manolio; C A McCarty; D A Nickerson; S E Scherer; M S Williams; D M Roden; J C Denny
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Review 5.  The Advantages and Challenges of Diversity in Pharmacogenomics: Can Minority Populations Bring Us Closer to Implementation?

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Review 6.  The Case for Pharmacogenetics-Guided Prescribing of Codeine in Children.

Authors:  Roseann S Gammal; Kelly E Caudle; Charles T Quinn; Winfred C Wang; Andrea Gaedigk; Cynthia A Prows; Cyrine E Haidar; Annette K Taylor; Teri E Klein; Katrin Sangkuhl; Jane S Hankins; Kristine R Crews
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Review 7.  Codeine and opioid metabolism: implications and alternatives for pediatric pain management.

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8.  Prior opioid exposure influences parents' sharing of their children's CYP2D6 research results.

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9.  Drug-gene and drug-drug interactions associated with tramadol and codeine therapy in the INGENIOUS trial.

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Review 10.  State of the Art Management of Acute Vaso-occlusive Pain in Sickle Cell Disease.

Authors:  Latika Puri; Kerri A Nottage; Jane S Hankins; Doralina L Anghelescu
Journal:  Paediatr Drugs       Date:  2018-02       Impact factor: 3.022

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