Wal-yan Respiratory Research Centre, Telethon Kids Institute, Perth, WA, Australia; Faculty of Health and Medical Sciences, University of Western Australia, Perth, WA, Australia; Department of Respiratory and Sleep Medicine, Perth Children's Hospital, Perth, WA, Australia.
Wal-yan Respiratory Research Centre, Telethon Kids Institute, Perth, WA, Australia.
Lancet Respir Med. 2022 Aug;10(8):776-784. doi: 10.1016/S2213-2600(22)00165-5. Epub 2022 Jun 2.
Structural lung disease and neutrophil-dominated airway inflammation is present from 3 months of age in children diagnosed with cystic fibrosis after newborn screening. We hypothesised that azithromycin, given three times weekly to infants with cystic fibrosis from diagnosis until age 36 months, would reduce the extent of structural lung disease as captured on chest CT scans.
A phase three, randomised, double-blind, placebo-controlled trial was done at eight paediatric cystic fibrosis centres in Australia and New Zealand. Infants (aged 3-6 months) diagnosed with cystic fibrosis following newborn screening were eligible. Exclusion criteria included prolonged mechanical ventilation in the first 3 months of life, clinically significant medical disease or comorbidities other than cystic fibrosis, or macrolide hypersensitivity. Participants were randomly assigned (1:1) to receive either azithromycin (10 mg/kg bodyweight orally three times per week) or matched placebo until age 36 months. Randomisation was done with a permuted block strategy and an interactive web-based response system, stratified by study site. Unblinding was done once all participants completed the trial. The two primary outcomes were the proportion of children with radiologically defined bronchiectasis, and the percentage of total lung volume affected by disease. Secondary outcomes included clinical outcomes and exploratory outcomes were inflammatory markers. Analyses were done with the intention-to-treat principle. This study is registered at ClinicalTrials.gov (NCT01270074).
Between June 15, 2012, and July 10, 2017, 281 patients were screened, of whom 130 were enrolled, randomly assigned, and received first study dose. 68 participants received azithromycin and 62 received placebo. At 36 months, 88% (n=50) of the azithromycin group and 94% (n=44) of the placebo group had bronchiectasis (odds ratio 0·49, 95% CI 0·12 to 2·00; p=0·32), and total airways disease did not differ between groups (median difference -0·02%, 95% CI -0·59 to 0·56; p=0·96). Secondary outcome results included fewer days in hospital for pulmonary exacerbations (mean difference -6·3, 95% CI -10·5 to -2·1; p=0·0037) and fewer courses of inhaled or oral antibiotics (incidence rate ratio 0·88, 95% CI 0·81 to 0·97; p=0·0088) for those in the azithromycin group. For the preplanned, exploratory analysis, concentrations of airway inflammation were lower for participants receiving azithromycin, including interleukin-8 (median difference -1·2 pg/mL, 95% CI -1·9 to -0·5; p=0·0012) and neutrophil elastase activity (-0·6 μg/mL, -1·1 to -0·2; p=0·0087) at age 36 months, although no difference was noted between the groups for interleukin-8 or neutrophil elastase activity at 12 months. There was no effect of azithromycin on body-mass index at age 36 months (mean difference 0·4, 95% CI -0·1 to 0·9; p=0·12), nor any evidence of pathogen emergence with the use of azithromycin. There were few adverse outcomes with no differences between the treatment groups.
Azithromycin treatment from diagnosis of cystic fibrosis did not reduce the extent of structural lung disease at 36 months of age; however, it did reduce airway inflammation, morbidity including pulmonary exacerbations in the first year of life and hospitalisations, and improved some clinical outcomes associated with cystic fibrosis lung disease. Therefore we suggest thrice-weekly azithromycin is a strategy that could be considered for the routine early management of paediatric patients with cystic fibrosis.
Cystic Fibrosis Foundation.
在通过新生儿筛查诊断为囊性纤维化的儿童中,从 3 个月大开始就存在结构性肺病和以中性粒细胞为主的气道炎症。我们假设,从诊断到 36 个月大,每周三次给予囊性纤维化婴儿阿奇霉素治疗,将减少胸部 CT 扫描上结构性肺病的程度。
在澳大利亚和新西兰的 8 个儿科囊性纤维化中心进行了一项 III 期、随机、双盲、安慰剂对照试验。符合条件的是在新生儿筛查后被诊断为囊性纤维化的婴儿(年龄 3-6 个月)。排除标准包括生命的前 3 个月中需要长时间机械通气、存在除囊性纤维化以外的临床显著疾病或合并症、或对大环内酯类药物过敏。参与者被随机分配(1:1)接受阿奇霉素(10mg/kg 体重口服,每周 3 次)或匹配的安慰剂,直到 36 个月大。随机分配采用了随机化块策略和交互式网络响应系统,按研究地点分层。一旦所有参与者完成试验,就进行双盲。两个主要结局是影像学定义的支气管扩张的比例,以及受疾病影响的总肺容量的百分比。次要结局包括临床结局和探索性结局,如炎症标志物。分析采用意向治疗原则。本研究在 ClinicalTrials.gov 注册(NCT01270074)。
2012 年 6 月 15 日至 2017 年 7 月 10 日期间,共有 281 名患者接受了筛查,其中 130 名被纳入研究,随机分配并接受了首次研究剂量。68 名参与者接受了阿奇霉素治疗,62 名接受了安慰剂治疗。在 36 个月时,阿奇霉素组有 88%(n=50)的患者和安慰剂组有 94%(n=44)的患者患有支气管扩张症(比值比 0·49,95%CI 0·12 至 2·00;p=0·32),两组总气道疾病无差异(中位数差异-0·02%,95%CI -0·59 至 0·56;p=0·96)。次要结局结果包括因肺部恶化而住院的天数减少(平均差异-6·3,95%CI -10·5 至 -2·1;p=0·0037)和吸入或口服抗生素的疗程减少(发病率比 0·88,95%CI 0·81 至 0·97;p=0·0088),阿奇霉素组的这些结果更好。对于预先计划的探索性分析,接受阿奇霉素治疗的参与者的气道炎症浓度较低,包括白细胞介素-8(中位数差异-1·2pg/ml,95%CI -1·9 至 -0·5;p=0·0012)和中性粒细胞弹性蛋白酶活性(-0·6μg/ml,-1·1 至 -0·2;p=0·0087),但在 12 个月时,两组之间的白细胞介素-8 或中性粒细胞弹性蛋白酶活性无差异。阿奇霉素治疗对 36 个月时的体重指数没有影响(平均差异 0·4,95%CI 0·1 至 0·9;p=0·12),也没有证据表明使用阿奇霉素会导致病原体出现。治疗组的不良结局很少,没有差异。
从囊性纤维化的诊断开始,阿奇霉素治疗并未在 36 个月时减少结构性肺病的程度;然而,它确实减少了气道炎症、发病率,包括生命第一年的肺部恶化和住院,以及改善了一些与囊性纤维化肺病相关的临床结局。因此,我们建议每周三次阿奇霉素是一种可以考虑用于囊性纤维化患儿常规早期管理的策略。
囊性纤维化基金会。
