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Organ and gestational age effects of maternal nutrient restriction on global methylation in fetal baboons
Authors:A. Unterberger,M. Szyf,P.W. Nathanielsz,&   L.A. Cox
Affiliation: Pharmacology and Therapeutics, McGill University, Montreal, Quebec, Canada;
 Southwest National Primate Research Center, Southwest Foundation for Biomedical Research, San Antonio, TX, USA;
 Center for Pregnancy and Newborn Research, Uthscsa, San Antonio, TX, USA;
 Department of Genetics, Southwest Foundation for Biomedical Research, San Antonio, TX, USA
Abstract:Background  A sub-optimal intrauterine environment alters the trajectory of fetal development with profound effects on life-time health. Altered methylation, a proposed epigenetic mechanism responsible for these changes, has been studied in non-primate species but not nonhuman primates. We tested the hypotheses that global methylation in fetal baboon demonstrates organ specificity, gestational age specificity, and changes with maternal nutritional status.
Methods  We measured global DNA methylation in fetuses of control fed (CTR) and nutrient restricted mothers fed 70% of controls (MNR) for brain, kidney, liver and heart at 0.5 and 0.9 gestation (G).
Results  We observed organ and gestation specific changes that were modified by maternal diet. Methylation in CTR fetuses was highest in frontal cortex and lowest in liver. MNR decreased methylation in 0.5G kidney and increased methylation in 0.9G kidney and frontal cortex.
Conclusion  These results demonstrate a potential epigenetic mechanism whereby reduced maternal nutrition has long-term programming effects on fetal organ development.
Keywords:development    nonhuman primate
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