4.4 Article

Maternal nicotinamide supplementation causes global DNA hypomethylation, uracil hypo-incorporation and gene expression changes in fetal rats

Journal

BRITISH JOURNAL OF NUTRITION
Volume 111, Issue 9, Pages 1594-1601

Publisher

CAMBRIDGE UNIV PRESS
DOI: 10.1017/S0007114513004054

Keywords

Epigenetic changes; Nicotinamide; DNA hypomethylation; Maternal nutrient supplementation

Funding

  1. National Natural Science Foundations of China [31140036, 81000575]
  2. Foundation of Key Laboratory of Education Department of Liaoning Province [L2012441]

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Recent evidence shows that excess nicotinamide can cause epigenetic changes in developing rats. The aim of the present study was to investigate the effects of maternal nicotinamide supplementation on the fetus. Female rats were randomised into four groups fed a standard chow diet (control group) or diets supplemented with 1g/kg of nicotinamide (low-dose group), 4g/kg of nicotinamide (high-dose group) or 4g/kg of nicotinamide plus 2g/kg of betaine (betaine group) for 14-16d before mating and throughout the study. Fetal tissue samples were collected on the 20th day of pregnancy. Compared with the control group, the high-dose group had a higher fetal death rate, and the average fetal body weight was higher in the low-dose group but lower in the high-dose group. Nicotinamide supplementation led to a decrease in placental and fetal hepatic genomic DNA methylation and genomic uracil contents (a factor modifying DNA for diversity) in the placenta and fetal liver and brain, which could be completely or partially prevented by betaine. Moreover, nicotinamide supplementation induced tissue-specific alterations in the mRNA expression of the genes encoding nicotinamide N-methyltransferase, DNA methyltransferase 1, catalase and tumour protein p53 in the placenta and fetal liver. High-dose nicotinamide supplementation increased fetal hepatic alpha-fetoprotein mRNA level, which was prevented by betaine supplementation. It is concluded that maternal nicotinamide supplementation can induce changes in fetal epigenetic modification and DNA base composition. The present study raises the concern that maternal nicotinamide supplementation may play a role in the development of epigenetic-related diseases in the offspring.

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