Darboe Momodou K, Thurnham David I, Morgan Gareth, Adegbola Richard A, Secka Ousman, Solon Juan A, Jackson Sarah J, Northrop-Clewes Christine, Fulford Tony J, Doherty Conor P, Prentice Andrew M
MRC International Nutrition Group, London School of Hygiene and Tropical Medicine, London, UK.
Lancet. 2007 Jun 23;369(9579):2088-96. doi: 10.1016/S0140-6736(07)60981-7.
Most developing countries have adopted a standard WHO dosing schedule for vitamin A supplementation. However, in 2002 the International Vitamin A Consultative Group (IVACG) Annecy Accord recommended a new high-dose regimen for mothers and infants. Our aim was to test whether the new high-dose regimen of vitamin A supplementation would increase maternal and infant plasma vitamin A, reduce infant Helicobacter pylori infection and nasopharyngeal pneumococcal carriage, and improve infant gut epithelial integrity.
In an area of moderate vitamin A deficiency in rural Gambia, 220 mother-infant pairs were enrolled in a randomised double-blind trial between September, 2001, and October, 2004, that compared the IVACG high dose with the WHO dose. The primary endpoints were levels of maternal and infant plasma vitamin A, H pylori infection, pneumococcal carriage, and gut epithelial integrity. The trial is registered as ISRCTN 98554309.
197 infants completed follow-up to 12 months (99 high dose and 98 WHO dose). There were no adverse events at dosing. No differences were found in the primary outcomes for high-dose versus WHO schedule: maternal vitamin A concentration at 2 months +0.02 micromol/L (95% CI -0.10 to 0.15); infant vitamin A at 5 months +0.01 micromol/L (-0.06 to 0.08); H pylori infection at 12 months -0.3% (-14.7 to 14.2); maternal pneumococcal carriage at 12 months -2.0% (-13.7 to 9.7); infant pneumococcal carriage at 12 months -4.1% (-15.8 to 7.6); infant gut mucosal damage at 12 months 5.2% (-8.7 to 19.2). There were more clinic attendances by the high-dose group in the first 6 months of life (p=0.018).
Our results do not lend support to the proposal to increase the existing WHO standard dosing schedule for vitamin A in areas of moderate vitamin A deficiency. Caution is urged for future studies because trials have shown possible adverse effects of higher doses of vitamin A, and potential negative interactions with the expanded programme on immunisation (EPI) vaccines.
大多数发展中国家已采用世界卫生组织(WHO)的维生素A补充标准剂量方案。然而,2002年国际维生素A咨询小组(IVACG)阿讷西协定推荐了一种针对母亲和婴儿的新的高剂量方案。我们的目的是测试维生素A补充的新高剂量方案是否会提高母婴血浆维生素A水平,减少婴儿幽门螺杆菌感染和鼻咽部肺炎球菌携带,并改善婴儿肠道上皮完整性。
在冈比亚农村维生素A中度缺乏的地区,220对母婴于2001年9月至2004年10月参加了一项随机双盲试验,比较了IVACG高剂量方案与WHO剂量方案。主要终点是母婴血浆维生素A水平、幽门螺杆菌感染、肺炎球菌携带情况和肠道上皮完整性。该试验已在国际标准随机对照试验编号库注册,编号为ISRCTN 98554309。
197名婴儿完成了12个月的随访(99名接受高剂量方案,98名接受WHO剂量方案)。给药时未出现不良事件。高剂量方案与WHO方案在主要结局方面未发现差异:2个月时母亲维生素A浓度为+0.02微摩尔/升(95%置信区间为-0.10至0.15);5个月时婴儿维生素A浓度为+0.01微摩尔/升(-0.06至0.08);12个月时幽门螺杆菌感染率为-0.3%(-14.7至14.2);12个月时母亲肺炎球菌携带率为-2.0%(-13.7至9.7);12个月时婴儿肺炎球菌携带率为-4.1%(-15.8至7.6);12个月时婴儿肠道黏膜损伤率为5.2%(-8.7至19.2)。高剂量组在生命的前6个月就诊次数更多(p=0.018)。
我们的结果不支持在维生素A中度缺乏地区增加现有WHO维生素A标准剂量方案的提议。鉴于试验已表明高剂量维生素A可能存在不良反应,以及与扩大免疫规划(EPI)疫苗可能存在负面相互作用,因此敦促未来的研究要谨慎。
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