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母体二十二碳六烯酸补充可减少高氧暴露新生小鼠的肺部炎症。

Maternal docosahexaenoic acid supplementation decreases lung inflammation in hyperoxia-exposed newborn mice.

机构信息

Center for Perinatal Research, The Ohio State University, Columbus, OH 43205, USA.

出版信息

J Nutr. 2011 Feb;141(2):214-22. doi: 10.3945/jn.110.129882. Epub 2010 Dec 22.

Abstract

DHA is a long-chain fatty acid that has potent antiinflammatory properties. Whereas maternal DHA dietary supplementation has been shown to improve cognitive development in infants fed DHA-supplemented milk, the antiinflammatory effects of maternal DHA supplementation on the developing fetus and neonate have not been extensively explored. Pregnant C3H/HeN dams were fed purified control or DHA-supplemented diets (~0.25% of total fat) at embryonic d 16 and consumed these diets throughout the study. At birth, the nursing mouse pups were placed in room air (RA; 21% O(2)) or >95% O(2) (hyperoxia) for up to 7 d. These studies tested the hypothesis that maternal DHA supplementation would decrease inflammation and improve alveolarization in the lungs of newborn mouse pups exposed to hyperoxia. Survival, inflammatory responses, and lung growth were compared among control diet/RA, DHA/RA, control/O(2), and DHA/O(2) pups. There were fewer neutrophils and macrophages in lung tissues from pups nursed by DHA-supplemented dams than in those nursed by dams fed the control diet at 7 d of hyperoxia exposure (P < 0.015). Although differences due to hyperoxia exposure were observed, maternal diet did not affect keratinocyte-derived chemokine, macrophage inflammatory protein-2, IL-1β, or TNFα mRNA levels in pup tissues. Hyperoxia also induced NF-κB activity, but maternal diet did not affect NF-κB or PPARγ activities. In mice, DHA supplementation decreases leukocyte infiltration in the offspring exposed to hyperoxia, suggesting a potential role for DHA supplementation as a therapy to reduce inflammation in preterm infants.

摘要

二十二碳六烯酸(DHA)是一种长链脂肪酸,具有很强的抗炎特性。虽然母体 DHA 膳食补充已被证明可以改善喂养 DHA 补充奶的婴儿的认知发育,但母体 DHA 补充对发育中胎儿和新生儿的抗炎作用尚未得到广泛探索。怀孕的 C3H/HeN 母鼠在胚胎第 16 天开始食用纯化的对照或 DHA 补充饮食(约占总脂肪的 0.25%),并在整个研究期间食用这些饮食。在出生时,哺乳的幼鼠被置于室内空气(RA;21%O2)或 >95%O2(高氧)中,持续 7 天。这些研究检验了这样一个假设,即母体 DHA 补充会减少暴露于高氧的新生幼鼠肺部的炎症并改善肺泡化。在接受对照饮食/RA、DHA/RA、对照/O2 和 DHA/O2 喂养的幼鼠中比较了存活率、炎症反应和肺生长。在高氧暴露 7 天时,由 DHA 补充的母鼠喂养的幼鼠的肺部组织中的中性粒细胞和巨噬细胞少于由对照饮食喂养的母鼠喂养的幼鼠(P<0.015)。尽管观察到了由于高氧暴露引起的差异,但母体饮食并未影响幼鼠组织中角质形成细胞衍生趋化因子、巨噬细胞炎症蛋白-2、IL-1β 或 TNFα 的 mRNA 水平。高氧也诱导了 NF-κB 活性,但母体饮食不影响 NF-κB 或 PPARγ 的活性。在小鼠中,DHA 补充可减少暴露于高氧的后代中的白细胞浸润,表明 DHA 补充作为治疗早产儿炎症的潜在作用。

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