Guenin Eric, Armogida Marianna, Riff Dennis
Novartis Consumer Health, Inc., Parsippany, NJ, USA,
Clin Drug Investig. 2014 Sep;34(9):609-16. doi: 10.1007/s40261-014-0210-5.
Dextromethorphan hydrobromide (DM) is a widely used antitussive. This study determined, for the first time, the basic pharmacokinetic profile of DM and its active metabolite, dextrorphan (DP) in children and adolescents.
Thirty-eight male and female subjects at risk for developing an upper respiratory tract infection (URTI), or symptomatic with cough due to URTI, were enrolled in this single-dose, open-label study: ages 2-5 years (Group A, n = 8), 6-11 years (Group B, n = 17), 12-17 years (Group C, n = 13). Subjects were genotyped for cytochrome P450 (CYP) 2D6 polymorphisms and characterized as poor (PM) or non-poor metabolizers (non-PM). Groups A and B were dosed using an age-weight dosing schedule (DM range 7.5-24.75 mg); a 30-mg dose was used for Group C.
Average exposures to total DP increased as age group increased, and average exposure to DM was highest in the adolescent group. One subject in that group was a PM. The terminal half-life (t ½) values were longer in the adolescent group due in part to the single PM subject. No relationship between body weight and pharmacokinetic parameters was noted.
This is the first evaluation of the pharmacokinetic characteristics of DM in children and adolescents. A single dose of DM in this population was safe, and well tolerated at all doses tested. The data are used to model and compare pediatric DM exposures with those of adults.
氢溴酸右美沙芬(DM)是一种广泛使用的止咳药。本研究首次确定了DM及其活性代谢物右啡烷(DP)在儿童和青少年中的基本药代动力学特征。
38名有发生上呼吸道感染(URTI)风险或因URTI出现咳嗽症状的男性和女性受试者参与了这项单剂量、开放标签研究:年龄2至5岁(A组,n = 8),6至11岁(B组,n = 17),12至17岁(C组,n = 13)。对受试者进行细胞色素P450(CYP)2D6基因多态性基因分型,并分为慢代谢者(PM)或非慢代谢者(非PM)。A组和B组采用年龄体重给药方案给药(DM剂量范围7.5至24.75 mg);C组使用30 mg剂量。
随着年龄组的增加,总DP的平均暴露量增加,青少年组中DM的平均暴露量最高。该组中有一名受试者为PM。青少年组的末端半衰期(t½)值较长,部分原因是有一名PM受试者。未观察到体重与药代动力学参数之间的关系。
这是首次对儿童和青少年中DM的药代动力学特征进行评估。该人群中单次剂量的DM是安全的,在所有测试剂量下耐受性良好。这些数据用于建立模型并比较儿童与成人的DM暴露情况。
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