4.7 Article

Gestational Iron Supplementation Improves Fetal Outcomes in a Rat Model of Prenatal Alcohol Exposure

期刊

NUTRIENTS
卷 14, 期 8, 页码 -

出版社

MDPI
DOI: 10.3390/nu14081653

关键词

prenatal alcohol exposure; iron deficiency; fetal anemia; iron supplementation; fer-in-sol; fetal growth; fetal brain development; rat iron requirement; feed conversion

资金

  1. National Institute of Health/National Institute on Alcohol Abuse and Alcoholism [R01 AA022999, R01 AA011085, K99 AA028291, F32 AA027121, F32 AA028684]
  2. National Institute on Diabetes and Digestive and Kidney Diseases [T32 DK007686]

向作者/读者索取更多资源

Prenatal alcohol exposure can cause neurodevelopmental disability and functional iron deficiency in the fetus. However, gestational administration of Fer-In-Sol, a clinically relevant iron supplement, can mitigate alcohol's adverse impacts on the fetus.
Prenatal alcohol exposure causes neurodevelopmental disability and is associated with a functional iron deficiency in the fetus and neonate, even when the mother consumes an apparently iron-adequate diet. Here, we test whether gestational administration of the clinically relevant iron supplement Fer-In-Sol mitigates alcohol's adverse impacts upon the fetus. Pregnant Long-Evans rats consumed an iron-adequate diet and received 5 g/kg alcohol by gavage for 7 days in late pregnancy. Concurrently, some mothers received 6 mg/kg oral iron. We measured maternal and fetal weights, hematology, tissue iron content, and oxidative damage on gestational day 20.5. Alcohol caused fetal anemia, decreased fetal body and brain weight, increased hepatic iron content, and modestly elevated hepatic malondialdehyde (p's < 0.05). Supplemental iron normalized this brain weight reduction in alcohol-exposed males (p = 0.154) but not female littermates (p = 0.031). Iron also reversed the alcohol-induced fetal anemia and normalized both red blood cell numbers and hematocrit (p's < 0.05). Iron had minimal adverse effects on the mother or fetus. These data show that gestational iron supplementation improves select fetal outcomes in prenatal alcohol exposure (PAE) including brain weight and hematology, suggesting that this may be a clinically feasible approach to improve prenatal iron status and fetal outcomes in alcohol-exposed pregnancies.

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