University of Bordeaux, National Institute for Health and Medical Research (INSERM), Research Institute for Sustainable Development (IRD), Bordeaux Population Health Centre, UMR 1219, Bordeaux, France.
The Alliance for International Medical Action (ALIMA), Paris, France.
Lancet Glob Health. 2022 Apr;10(4):e510-e520. doi: 10.1016/S2214-109X(22)00041-9.
Global access to acute malnutrition treatment is low. Different programmes using different nutritional products manage cases of severe acute malnutrition and moderate acute malnutrition separately. We aimed to assess whether integrating severe acute malnutrition and moderate acute malnutrition treatment into one programme, using a single nutritional product and reducing the dose as the child improves, could achieve similar or higher individual efficacy, increase coverage, and minimise costs compared with the current programmes.
We conducted an open-label, non-inferiority, randomised controlled trial in the Democratic Republic of the Congo. Acutely malnourished children aged 6-59 months with a mid-upper-arm circumference (MUAC) of less than 125 mm or oedema were randomly assigned (1:1), using specially developed software and random blocks (size was kept confidential), to either the current standard strategy (one programme for severe acute malnutrition using ready-to-use therapeutic food [RUTF] at an increasing dose as weight increased, another for moderate acute malnutrition using a fixed dose of ready-to-use supplementary food [RUSF]) or the OptiMA strategy (a single programme for both severe acute malnutrition and moderate acute malnutrition using RUTF at a decreasing dose as MUAC and weight increased). The primary endpoint was a favourable outcome at 6 months, defined as being alive, not acutely malnourished as per the definition applied at inclusion, and with no further episodes of acute malnutrition throughout the 6-month observation period; the endpoint was analysed in the intention-to-treat (all children) and per-protocol populations (participants who had a minimum prescription of 4 weeks' RUTF, received at least 90% of the total amount of RUTF they were supposed to receive as per the protocol, or were prescribed RUSF rations for a minimum of 4 weeks [ie, minimum of 28 RUSF sachets], and had a maximum interval of 6 weeks between any two visits in the 6-month follow-up). The non-inferiority analysis (margin 10%) was to be followed by a superiority analysis (margin 0%) if non-inferiority was concluded. This trial is registered at ClinicalTrials.gov, NCT03751475, and is now closed.
Between July 22 and Dec 6, 2019, 912 children were randomly assigned; after 16 were excluded, 896 were analysed (446 in the standard group and 450 in the OptiMA group). In the intention-to-treat analysis, 282 (63%) of 446 children in the standard group and 325 (72%) of 450 children in the OptiMA group had a favourable outcome (difference -9·0%, 95% CI -15·9 to -2·0). In the per protocol analysis, 161 (61%) of 264 children in the standard group and 291 (74%) of 392 children in the OptiMA group had a favourable outcome (-13·2%, -21·6 to -4·9).
In this non-inferiority trial treating children with MUAC of less than 125 mm or oedema, decreasing RUTF dose according to MUAC and weight increase proved to be a superior strategy to the standard protocol in the Democratic Republic of the Congo. These results demonstrate the safety and benefits of an approach that could substantially increase access to treatment for millions of children with acute malnutrition in sub-Saharan Africa.
Innocent Foundation and European Civil Protection and Humanitarian Aid Operations.
For the French translation of the abstract see Supplementary Materials section.
全球获得急性营养不良治疗的机会很低。不同的方案使用不同的营养产品分别管理严重急性营养不良和中度急性营养不良病例。我们旨在评估将严重急性营养不良和中度急性营养不良治疗整合到一个方案中,使用单一营养产品并随着儿童的改善减少剂量,是否可以实现类似或更高的个体疗效,增加覆盖率,并最大限度地降低成本与当前方案相比。
我们在刚果民主共和国进行了一项开放性、非劣效性、随机对照试验。患有急性营养不良的 6-59 个月大的儿童,其上臂中部周长(MAC)小于 125 毫米或有水肿,随机分配(1:1),使用专门开发的软件和随机块(大小保密),分为当前标准策略(一种用于严重急性营养不良的方案,使用递增剂量的即用型治疗食品[RUTF],随着体重增加;另一种用于中度急性营养不良的方案,使用固定剂量的即用型补充食品[RUSF])或 OptiMA 策略(一种用于严重急性营养不良和中度急性营养不良的单一方案,使用 RUTF 递减剂量,随着 MAC 和体重增加)。主要终点是 6 个月时的良好结局,定义为存活、根据纳入时应用的定义不患有急性营养不良、且在 6 个月观察期内无进一步急性营养不良发作;终点在意向治疗(所有儿童)和方案人群(接受至少 4 周 RUTF 处方、至少接受 90%按方案规定应接受的 RUTF 总量、或至少接受 4 周 RUSF 配给[即至少 28 个 RUSF 小袋],且在 6 个月随访期间任何两次就诊之间的最大间隔为 6 周)中进行分析。如果得出非劣效性结论,则将进行非劣效性分析(10%的边缘),然后进行优效性分析(0%的边缘)。该试验在 ClinicalTrials.gov 上注册,编号为 NCT03751475,现已关闭。
2019 年 7 月 22 日至 12 月 6 日期间,随机分配了 912 名儿童;排除 16 名后,对 896 名儿童进行了分析(标准组 446 名,OptiMA 组 450 名)。意向治疗分析中,标准组 446 名儿童中有 282 名(63%),OptiMA 组 450 名儿童中有 325 名(72%)有良好结局(差异-9.0%,95%CI-15.9 至-2.0)。在方案人群分析中,标准组 264 名儿童中有 161 名(61%),OptiMA 组 392 名儿童中有 291 名(74%)有良好结局(-13.2%,-21.6 至-4.9)。
在这项针对 MAC 小于 125 毫米或有水肿的儿童的非劣效性试验中,根据 MAC 和体重增加减少 RUTF 剂量被证明是一种优于刚果民主共和国标准方案的策略。这些结果证明了这种方法的安全性和益处,这种方法可以大大增加撒哈拉以南非洲数百万急性营养不良儿童获得治疗的机会。
无辜基金会和欧洲民防和人道主义援助行动。
