Literature DB >> 9057784

Pharmacogenetics in pediatrics. Implications for practice.

J S Leeder1, G L Kearns.   

Abstract

Cumulative experience with pharmacotherapy in children indicates that it is difficult to prescribe medications rationally solely on the basis of patient age. Furthermore, the apparent drug biotransformation phenotype may be influenced by disease (e.g., infection), environmental factors (e.g., diet and environmental contaminants), and concurrent medications. Therefore, characterization of drug biotransformation pathways during development and, at a given developmental stage, the effects of known modulators of drug biotransformation are essential for optimum treatment. This is particularly true when one considers that altered drug biotransformation may contribute significantly to therapeutic failure (e.g., graft rejection with inadequate serum and tissue concentrations of cyclosporin and myelotoxicity consequent to a relative inability to metabolize normal doses of certain antineoplastic agents). Accordingly, the goals of coordinated clinical and basic investigations should be to characterize important drug biotransformation pathways for compounds under development and intended for use in pediatrics and to identify the population extremes or "outliers" to aid in selection of an appropriate dosage range for efficacy studies. Acquired knowledge should then be incorporated into the drug-design process to further maximize the efficacy-toxicity ratio. The development of acceptable, preferably noninvasive, phenotyping procedures for all age ranges including neonates, infants, and older children is a major challenge for investigators but, if met, will be rewarded with improved pediatric pharmacotherapy.

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Year:  1997        PMID: 9057784     DOI: 10.1016/s0031-3955(05)70463-6

Source DB:  PubMed          Journal:  Pediatr Clin North Am        ISSN: 0031-3955            Impact factor:   3.278


  30 in total

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2.  Population pharmacokinetics of levamisole in children with steroid-sensitive nephrotic syndrome.

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Review 3.  Clinical pharmacology in the adolescent oncology patient.

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Review 4.  Cytochrome P450 3A: ontogeny and drug disposition.

Authors:  S N de Wildt; G L Kearns; J S Leeder; J N van den Anker
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5.  Cardiac Collapse Secondary to Phenytoin Toxicity in a Neonate Treated with Extracorporeal Membrane Oxygenation Support (ECMO).

Authors:  Michelle Knecht; Joseph LaRochelle; Brian Barkemeyer; Raegan Gupta; Michael Brumund; Christy Mumphrey
Journal:  J Med Toxicol       Date:  2019-11-26

Review 6.  Future pharmacologic agents for treatment of heart failure in children.

Authors:  Brady S Moffett; Anthony C Chang
Journal:  Pediatr Cardiol       Date:  2006-08-23       Impact factor: 1.655

7.  Pharmacokinetics of dapsone administered daily and weekly in human immunodeficiency virus-infected children.

Authors:  M Mirochnick; E Cooper; K McIntosh; J Xu; J Lindsey; D Jacobus; L Mofenson; J L Sullivan; W Dankner; L M Frenkel; S Nachman; D W Wara; D Johnson; V R Bonagura; M H Rathore; C K Cunningham; J McNamara
Journal:  Antimicrob Agents Chemother       Date:  1999-11       Impact factor: 5.191

Review 8.  Maternal-fetal transport of hypoglycaemic drugs.

Authors:  Facundo Garcia-Bournissen; Denice S Feig; Gideon Koren
Journal:  Clin Pharmacokinet       Date:  2003       Impact factor: 6.447

Review 9.  The adverse cardiac effects of Di(2-ethylhexyl)phthalate and Bisphenol A.

Authors:  Nikki Gillum Posnack
Journal:  Cardiovasc Toxicol       Date:  2014-12       Impact factor: 3.231

10.  Unusual presentation of iatrogenic phenytoin toxicity in a newborn.

Authors:  Jennifer A Lowry; John C Vandover; Jan DeGreeff; Anthony J Scalzo
Journal:  J Med Toxicol       Date:  2005-12
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