4 research outputs found

    The effect of amino acid deprivation on the transfer of iron through Caco-2 cell monolayers

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    Funding Source Rural and Environmental Scientific and Analytical Services, the Scottish Government Acknowledgments We thank Dr Helen Hayes for her technical support during this project. We also thank Dr Christine Kennedy for her involvement at the beginning of this project. This study was funded by Rural and Environmental Scientific and Advisory Service of Scottish Government.Peer reviewedPostprin

    The effect of maternal iron deficiency on zinc and copper levels and on genes of zinc and copper metabolism during pregnancy in the rat

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    Fe deficiency is relatively common in pregnancy and has both short- and long-term consequences. However, little is known about the effect on the metabolism of other micronutrients. A total of fifty-four female rats were fed control (50 mg Fe/kg) or Fe-deficient diets (7路5 mg/kg) before and during pregnancy. Maternal liver, placenta and fetal liver were collected at day 21 of pregnancy for Cu and Zn analysis and to measure expression of the major genes of Cu and Zn metabolism. Cu levels increased in the maternal liver (P=0路002) and placenta (P=0路018) of Fe-deficient rats. Zn increased (P&lt;0路0001) and Cu decreased (P=0路006) in the fetal liver. Hepatic expression of the Cu chaperones antioxidant 1 Cu chaperone (P=0路042) and cytochrome c oxidase Cu chaperone (COX17, P=0路020) decreased in the Fe-deficient dams, while the expression of the genes of Zn metabolism was unaltered. In the placenta, Fe deficiency reduced the expression of the chaperone for superoxide dismutase 1, Cu chaperone for superoxide dismutase (P=0路030), ceruloplasmin (P=0路042) and Zn transport genes, ZRT/IRT-like protein 4 (ZIP4, P=0路047) and Zn transporter 1 (ZnT1, P=0路012). In fetal liver, Fe deficiency increased COX17 (P=0路020), ZRT/IRT-like protein 14 (P=0路036) and ZnT1 (P=0路0003) and decreased ZIP4 (P=0路004). The results demonstrate that Fe deficiency during pregnancy has opposite effects on Cu and Zn levels in the fetal liver. This may, in turn, alter metabolism of these nutrients, with consequences for development in the fetus and the neonate.</p
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