利福平耐药性结核病患儿中可分散片剂莫西沙星的群体药代动力学及给药方案
Population pharmacokinetics and dosing of dispersible moxifloxacin formulation in children with rifampicin-resistant tuberculosis.
作者信息
Palmer Megan, Zou Yuanxi, Hesseling Anneke C, van der Laan Louvina, Courtney Ingrid, Kinikar Aarti A, Sonkawade Naresh, Paradkar Mandar, Kulkarni Vandana, Casalme Dessa Jean O, Frias Melchor V G, Draper Heather, Wiesner Lubbe, Karlsson Mats O, Denti Paolo, Svensson Elin M, Garcia-Prats Anthony J
机构信息
Desmond Tutu TB Centre, Department of Paediatrics and Child Health, Stellenbosch University, Cape Town, South Africa.
Department of Pharmacy, Uppsala University, Uppsala, Sweden.
出版信息
Br J Clin Pharmacol. 2025 Jun;91(6):1853-1864. doi: 10.1111/bcp.70005.
AIMS
Moxifloxacin is a priority drug for treating rifampicin-resistant tuberculosis (RR-TB). We assessed the pharmacokinetics of a child-friendly, dispersible 100 mg tablet moxifloxacin formulation (dispersed in water) compared to the standard 400 mg non-dispersible formulation (crushed and suspended in water) in children and evaluated current dosing recommendations.
METHODS
The CATALYST trial investigated the pharmacokinetics of moxifloxacin in children with RR-TB. Children were enrolled in South Africa, India and the Philippines. Intensive pharmacokinetic sampling was undertaken while children were taking the standard non-dispersible 400 mg moxifloxacin tablet formulation and repeated after switching to the novel dispersible formulation. Pharmacokinetic data were analysed using population pharmacokinetic modelling. Simulations were performed to evaluate moxifloxacin exposures in children compared to consensus adult reference exposures using current World Health Organization (WHO)-recommended doses and more recent model-based doses.
RESULTS
Thirty-six children were enrolled [median age 4.8 (range 0.4-15) years and weight 15.6 (range 6.9-42.1) kg]. A two-compartment disposition model with first-order elimination and delayed absorption was developed. The bioavailability of dispersible versus standard formulations fulfilled standard bioequivalence criterion (ratio 1.05 with 90% confidence interval 0.95-1.15). Simulations showed WHO-recommended doses achieved exposures similar to those in adults in children >10 kg, while children <10 kg may require 33%-56% higher doses to reach adult reference exposures.
CONCLUSIONS
Dosing recommendations for children can be the same for the dispersible paediatric and standard non-dispersible adult moxifloxacin formulation. The current WHO dosing recommendation risks underdosing moxifloxacin in children <10 kg. We propose optimized moxifloxacin doses for both formulations.
目的
莫西沙星是治疗耐利福平结核病(RR-TB)的重点药物。我们评估了一种适合儿童的100毫克可分散片剂莫西沙星制剂(分散于水中)与标准400毫克不可分散片剂(碾碎后悬浮于水中)在儿童体内的药代动力学,并对当前的给药建议进行了评估。
方法
CATALYST试验研究了莫西沙星在RR-TB儿童中的药代动力学。儿童在南非、印度和菲律宾入组。在儿童服用标准400毫克不可分散片剂莫西沙星制剂时进行密集药代动力学采样,并在换用新型可分散片剂后重复采样。使用群体药代动力学模型分析药代动力学数据。进行模拟以评估与使用世界卫生组织(WHO)当前推荐剂量及更新的基于模型的剂量的成人共识参考暴露量相比,儿童体内莫西沙星的暴露情况。
结果
36名儿童入组[中位年龄4.8(范围0.4 - 15)岁,体重15.6(范围6.9 - 42.1)千克]。建立了具有一级消除和延迟吸收的二室处置模型。可分散片剂与标准制剂的生物利用度符合标准生物等效性标准(比值为1.05,90%置信区间为0.95 - 1.15)。模拟显示,WHO推荐剂量在体重>10千克的儿童中实现的暴露量与成人相似,而体重<10千克的儿童可能需要高33% - 56%的剂量才能达到成人参考暴露量。
结论
可分散儿科剂型和标准不可分散成人剂型的莫西沙星给药建议对儿童可以相同。WHO当前的给药建议有使体重<10千克的儿童莫西沙星剂量不足的风险。我们提出了两种制剂的优化莫西沙星剂量。
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