Pediatric Infectious Diseases Research Group, Medical Research Council Clinical Trial Unit at University College London, Institute for Infection and Immunity, St George's University of London, London, United Kingdom.
Medical Research Council Clinical Trials Unit at University College London, London, United Kingdom.
JAMA. 2021 Nov 2;326(17):1713-1724. doi: 10.1001/jama.2021.17843.
The optimal dose and duration of oral amoxicillin for children with community-acquired pneumonia (CAP) are unclear.
To determine whether lower-dose amoxicillin is noninferior to higher dose and whether 3-day treatment is noninferior to 7 days.
DESIGN, SETTING, AND PARTICIPANTS: Multicenter, randomized, 2 × 2 factorial noninferiority trial enrolling 824 children, aged 6 months and older, with clinically diagnosed CAP, treated with amoxicillin on discharge from emergency departments and inpatient wards of 28 hospitals in the UK and 1 in Ireland between February 2017 and April 2019, with last trial visit on May 21, 2019.
Children were randomized 1:1 to receive oral amoxicillin at a lower dose (35-50 mg/kg/d; n = 410) or higher dose (70-90 mg/kg/d; n = 404), for a shorter duration (3 days; n = 413) or a longer duration (7 days; n = 401).
The primary outcome was clinically indicated antibiotic re-treatment for respiratory infection within 28 days after randomization. The noninferiority margin was 8%. Secondary outcomes included severity/duration of 9 parent-reported CAP symptoms, 3 antibiotic-related adverse events, and phenotypic resistance in colonizing Streptococcus pneumoniae isolates.
Of 824 participants randomized into 1 of the 4 groups, 814 received at least 1 dose of trial medication (median [IQR] age, 2.5 years [1.6-2.7]; 421 [52%] males and 393 [48%] females), and the primary outcome was available for 789 (97%). For lower vs higher dose, the primary outcome occurred in 12.6% with lower dose vs 12.4% with higher dose (difference, 0.2% [1-sided 95% CI -∞ to 4.0%]), and in 12.5% with 3-day treatment vs 12.5% with 7-day treatment (difference, 0.1% [1-sided 95% CI -∞ to 3.9]). Both groups demonstrated noninferiority with no significant interaction between dose and duration (P = .63). Of the 14 prespecified secondary end points, the only significant differences were 3-day vs 7-day treatment for cough duration (median 12 days vs 10 days; hazard ratio [HR], 1.2 [95% CI, 1.0 to 1.4]; P = .04) and sleep disturbed by cough (median, 4 days vs 4 days; HR, 1.2 [95% CI, 1.0 to 1.4]; P = .03). Among the subgroup of children with severe CAP, the primary end point occurred in 17.3% of lower-dose recipients vs 13.5% of higher-dose recipients (difference, 3.8% [1-sided 95% CI, -∞ to10%]; P value for interaction = .18) and in 16.0% with 3-day treatment vs 14.8% with 7-day treatment (difference, 1.2% [1-sided 95% CI, -∞ to 7.4%]; P value for interaction = .73).
Among children with CAP discharged from an emergency department or hospital ward (within 48 hours), lower-dose outpatient oral amoxicillin was noninferior to higher dose, and 3-day duration was noninferior to 7 days, with regard to need for antibiotic re-treatment. However, disease severity, treatment setting, prior antibiotics received, and acceptability of the noninferiority margin require consideration when interpreting the findings.
ISRCTN Identifier: ISRCTN76888927.
重要性:儿童社区获得性肺炎(CAP)的最佳口服阿莫西林剂量和持续时间尚不清楚。
目的:确定低剂量阿莫西林是否不劣于高剂量,以及 3 天疗程是否不劣于 7 天疗程。
设计、地点和参与者:这项多中心、随机、2×2 因子非劣效性试验纳入了 2017 年 2 月至 2019 年 4 月期间英国 28 家医院和爱尔兰 1 家医院的急诊科和住院病房中,824 名年龄在 6 个月及以上、临床诊断为 CAP 的儿童,在出院时接受阿莫西林治疗,试验于 2019 年 5 月 21 日最后一次访视。
干预措施:儿童随机 1:1 接受口服阿莫西林低剂量(35-50mg/kg/d;n=410)或高剂量(70-90mg/kg/d;n=404),疗程较短(3 天;n=413)或较长(7 天;n=401)。
主要结果和措施:主要结局是随机分组后 28 天内再次因呼吸道感染而接受临床指示的抗生素治疗。非劣效性边界为 8%。次要结局包括 9 项父母报告的 CAP 症状的严重程度/持续时间、3 项抗生素相关不良事件和定植性肺炎链球菌分离株的表型耐药性。
结果:824 名参与者随机分为 4 组中的 1 组,814 名至少接受了 1 剂试验药物(中位数[IQR]年龄,2.5 岁[1.6-2.7];421[52%]为男性,393[48%]为女性),789 名(97%)可获得主要结局。与高剂量相比,低剂量组和高剂量组的主要结局发生率分别为 12.6%和 12.4%(差异,0.2%[1 侧 95%CI-∞至 4.0%]),3 天疗程组和 7 天疗程组的主要结局发生率分别为 12.5%和 12.5%(差异,0.1%[1 侧 95%CI-∞至 3.9%])。两组均表现出非劣效性,剂量和持续时间之间无显著交互作用(P=0.63)。在 14 个预先指定的次要终点中,仅咳嗽持续时间(中位数 12 天 vs 10 天;危险比[HR],1.2[95%CI,1.0 至 1.4];P=0.04)和咳嗽引起的睡眠障碍(中位数 4 天 vs 4 天;HR,1.2[95%CI,1.0 至 1.4];P=0.03)存在显著差异。在 CAP 严重程度的亚组中,低剂量组的主要结局发生率为 17.3%,高剂量组为 13.5%(差异,3.8%[1 侧 95%CI-∞至 10%];P 值用于交互作用=0.18),3 天疗程组为 16.0%,7 天疗程组为 14.8%(差异,1.2%[1 侧 95%CI-∞至 7.4%];P 值用于交互作用=0.73)。
结论和相关性:在急诊科或病房(48 小时内)出院的 CAP 患儿中,低剂量门诊口服阿莫西林不劣于高剂量,3 天疗程不劣于 7 天疗程,在需要抗生素再次治疗方面。然而,疾病严重程度、治疗环境、之前使用的抗生素和非劣效性边界的可接受性需要在解释研究结果时加以考虑。
试验注册:ISRCTN 标识符:ISRCTN76888927。
