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一种用于严重急性营养不良住院儿童稳定的低碳水化合物和无乳糖配方:一项双盲、随机对照试验。

A reduced-carbohydrate and lactose-free formulation for stabilization among hospitalized children with severe acute malnutrition: A double-blind, randomized controlled trial.

机构信息

Division of Gastroenterology, Hepatology and Nutrition, Hospital for Sick Children, Toronto, Canada.

Translational Medicine Program, Hospital for Sick Children, Toronto, Canada.

出版信息

PLoS Med. 2019 Feb 26;16(2):e1002747. doi: 10.1371/journal.pmed.1002747. eCollection 2019 Feb.

Abstract

BACKGROUND

Children with medically complicated severe acute malnutrition (SAM) have high risk of inpatient mortality. Diarrhea, carbohydrate malabsorption, and refeeding syndrome may contribute to early mortality and delayed recovery. We tested the hypothesis that a lactose-free, low-carbohydrate F75 milk would serve to limit these risks, thereby reducing the number of days in the stabilization phase.

METHODS AND FINDINGS

In a multicenter double-blind trial, hospitalized severely malnourished children were randomized to receive standard formula (F75) or isocaloric modified F75 (mF75) without lactose and with reduced carbohydrate. The primary endpoint was time to stabilization, as defined by the World Health Organization (WHO), with intention-to-treat analysis. Secondary outcomes included in-hospital mortality, diarrhea, and biochemical features of malabsorption and refeeding syndrome. The trial was registered at clinicaltrials.gov (NCT02246296). Four hundred eighteen and 425 severely malnourished children were randomized to F75 and mF75, respectively, with 516 (61%) enrolled in Kenya and 327 (39%) in Malawi. Children with a median age of 16 months were enrolled between 4 December 2014 and 24 December 2015. One hundred ninety-four (46%) children assigned to F75 and 188 (44%) to mF75 had diarrhea at admission. Median time to stabilization was 3 days (IQR 2-5 days), which was similar between randomized groups (0.23 [95% CI -0.13 to 0.60], P = 0.59). There was no evidence of effect modification by diarrhea at admission, age, edema, or HIV status. Thirty-six and 39 children died before stabilization in the F75 and in mF75 arm, respectively (P = 0.84). Cumulative days with diarrhea (P = 0.27), enteral (P = 0.42) or intravenous fluids (P = 0.19), other serious adverse events before stabilization, and serum and stool biochemistry at day 3 did not differ between groups. The main limitation was that the primary outcome of clinical stabilization was based on WHO guidelines, comprising clinical evidence of recovery from acute illness as well as metabolic stabilization evidenced by recovery of appetite.

CONCLUSIONS

Empirically treating hospitalized severely malnourished children during the stabilization phase with lactose-free, reduced-carbohydrate milk formula did not improve clinical outcomes. The biochemical analyses suggest that the lactose-free formulae may still exceed a carbohydrate load threshold for intestinal absorption, which may limit their usefulness in the context of complicated SAM.

TRIAL REGISTRATION

ClinicalTrials.gov NCT02246296.

摘要

背景

患有医学上复杂的严重急性营养不良 (SAM) 的儿童住院死亡率较高。腹泻、碳水化合物吸收不良和再喂养综合征可能导致早期死亡和恢复延迟。我们检验了这样一个假设,即无乳糖、低碳水化合物 F75 奶可用于限制这些风险,从而减少稳定期的天数。

方法和发现

在一项多中心、双盲试验中,住院严重营养不良的儿童被随机分配接受标准配方 (F75) 或等热量改良 F75 (mF75),不添加乳糖且碳水化合物含量降低。主要终点是根据世界卫生组织 (WHO) 的定义达到稳定,采用意向治疗分析。次要结局包括住院死亡率、腹泻以及吸收不良和再喂养综合征的生化特征。该试验在 clinicaltrials.gov 上注册(NCT02246296)。418 名和 425 名严重营养不良的儿童分别随机分配到 F75 和 mF75,其中 516 名(61%)在肯尼亚入组,327 名(39%)在马拉维入组。儿童的中位年龄为 16 个月,入组时间为 2014 年 12 月 4 日至 2015 年 12 月 24 日。194 名(46%)分配到 F75 的儿童和 188 名(44%)分配到 mF75 的儿童入院时均有腹泻。稳定期中位数为 3 天(IQR 2-5 天),随机分组间相似(0.23 [95%CI -0.13 至 0.60],P=0.59)。入院时腹泻、年龄、水肿或 HIV 状态无证据表明存在效应修饰。在 F75 和 mF75 臂中,分别有 36 名和 39 名儿童在稳定化前死亡(P=0.84)。在稳定化前,腹泻(P=0.27)、肠内(P=0.42)或静脉输液(P=0.19)天数、其他严重不良事件以及第 3 天的血清和粪便生化指标在两组间无差异。主要限制是临床稳定的主要结局是基于世卫组织的指南,包括急性疾病恢复的临床证据以及通过食欲恢复证明代谢稳定。

结论

在稳定期,对住院严重营养不良的儿童进行经验性治疗,使用无乳糖、低碳水化合物奶配方并未改善临床结局。生化分析表明,无乳糖配方可能仍超过肠道吸收的碳水化合物负荷阈值,这可能限制了它们在复杂 SAM 情况下的应用。

试验注册

ClinicalTrials.gov NCT02246296。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9c6/6390989/9a27934b1358/pmed.1002747.g001.jpg

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