Desmond Tutu TB Centre, Department of Paediatrics and Child Health, Faculty of Medicine and Health Sciences, Stellenbosch Universitygrid.11956.3a, Cape Town, South Africa.
De La Salle Health Science Center, Cavite, Philippines.
Antimicrob Agents Chemother. 2022 May 17;66(5):e0214421. doi: 10.1128/aac.02144-21. Epub 2022 Apr 11.
Delamanid has been demonstrated to be safe and effective for treatment of adult multidrug-resistant tuberculosis (MDR-TB) and has been approved by the European Commission for treatment of pediatric MDR-TB patients at least 10 kg in weight, making the drug no longer limited to adults. A 10-day phase I age deescalation study was conducted, followed by a 6-month phase II extension study, to assess the pharmacokinetics, safety, tolerability, and preliminary efficacy of delamanid when combined with optimized background regimen (OBR) in children (birth to 17 years) with MDR-TB. Delamanid administered at 100 mg twice-daily (BID), 50 mg BID, and 25 mg BID resulted in exposures in 12- to 17- ( = 7), 6- to 11- ( = 6), and 3- to 5-year-olds ( = 12), respectively, comparable with those in adults at the approved adult dosage (100 mg BID). Exposures in 0- to 2-year-olds ( = 12) following a weight-based dosing regimen (5 mg once daily [QD] to 10 mg BID) were lower than predicted from pharmacokinetic modeling of the older three age groups and below target exposures in adults. Overall, the safety profile of delamanid in children 0 to 17 years of age was similar to the adult profile. At 24 months after the first delamanid dose, 33/37 children (89.2%) had favorable treatment outcomes, as defined by the World Health Organization (15/37 [40.5%] cured and 18/37 [48.6%] completed treatment). A new pediatric delamanid formulation used in 0- to 2-year-olds and 3- to 5-year-olds was palatable per child/parent and nurse/investigator reports. Data from initial phase I/II studies inform our understanding of delamanid use in children and support its further assessment in the setting of pediatric MDR-TB. (This study has been registered at ClinicalTrials.gov under identifiers NCT01856634 [phase I trial] and NCT01859923 [phase II trial].).
德拉马尼已被证明可安全有效地治疗成人耐多药结核病(MDR-TB),并已获得欧洲委员会批准,可用于治疗至少 10 公斤重的儿科 MDR-TB 患者,这使得该药物不再仅限于成人使用。进行了一项为期 10 天的 I 期年龄逐步降低研究,随后进行了一项为期 6 个月的 II 期扩展研究,以评估德拉马尼联合优化背景治疗方案(OBR)在患有 MDR-TB 的儿童(出生至 17 岁)中的药代动力学、安全性、耐受性和初步疗效。100mg 每日两次(BID)、50mg BID 和 25mg BID 的剂量分别使 12 至 17 岁( = 7)、6 至 11 岁( = 6)和 3 至 5 岁儿童( = 12)的暴露量与成人批准的成人剂量(100mg BID)相当。根据对年龄较大的三个年龄组的药代动力学模型进行预测,0 至 2 岁儿童( = 12)接受基于体重的剂量方案(每天 5mg 一次 [QD]至 10mg BID)后的暴露量低于预期,且低于成人的目标暴露量。总体而言,0 至 17 岁儿童使用德拉马尼的安全性与成人相似。在首次服用德拉马尼后 24 个月,37 名儿童中有 33 名(89.2%)达到了世界卫生组织(WHO)的良好治疗结局定义(15 名[40.5%]治愈,18 名[48.6%]完成治疗)。用于 0 至 2 岁和 3 至 5 岁儿童的新型儿科德拉马尼制剂,根据儿童/家长和护士/研究者的报告,口感良好。来自 I 期/II 期初步研究的数据使我们对儿童使用德拉马尼的情况有了进一步的了解,并支持在儿科 MDR-TB 背景下进一步评估。(该研究已在 ClinicalTrials.gov 上注册,标识符为 NCT01856634[I 期试验]和 NCT01859923[II 期试验])。
