4.7 Article

Genetic Variants in One-Carbon Metabolism and Their Effects on DHA Biomarkers in Pregnant Women: A Post-Hoc Analysis

期刊

NUTRIENTS
卷 14, 期 18, 页码 -

出版社

MDPI
DOI: 10.3390/nu14183801

关键词

choline; DHA; pregnancy; genetic variants; one-carbon metabolism; PEMT

资金

  1. Balchem Corporation
  2. Cornell Institute of Biotechnology's Center for Advanced Technology (CAT) grant through New York State Division of Science, Technology, and Innovation (NYSTAR)
  3. National Institute of Food and Agriculture US Department of Agriculture (NIFA/USDA), HATCH [1013729]
  4. NIH Training Grant [T32HD087137, T32ES027801]

向作者/读者索取更多资源

This study investigated the impact of genetic variants in one-carbon metabolism genes on DHA status, and found that genotype may influence maternal and fetal DHA levels, highlighting the importance of considering genetic variants in one-carbon metabolic genes during pregnancy.
The delivery of docosahexanoic acid (DHA) to the fetus is dependent on maternal one-carbon metabolism, as the latter supports the hepatic synthesis and export of a DHA-enriched phosphatidylcholine molecule via the phosphatidylethanolamine N-methyltransferase (PEMT) pathway. The following is a post-hoc analysis of a choline intervention study that sought to investigate whether common variants in one-carbon metabolizing genes associate with maternal and/or fetal blood biomarkers of DHA status. Pregnant women entering their second trimester were randomized to consume, until delivery, either 25 (n = 15) or 550 (n = 15) mg choline/d, and the effects of genetic variants in the PEMT, BHMT, MTHFD1, and MTHFR genes on DHA status were examined. Variant (vs. non-variant) maternal PEMT rs4646343 genotypes tended to have lower maternal RBC DHA (% total fatty acids) throughout gestation (6.9% vs. 7.4%; main effect, p = 0.08) and lower cord RBC DHA at delivery (7.6% vs. 8.4%; main effect, p = 0.09). Conversely, variant (vs. non-variant) maternal MTHFD1 rs2235226 genotypes exhibited higher cord RBC DHA (8.3% vs. 7.3%; main effect, p = 0.0003) and higher cord plasma DHA (55 vs. 41 mu g/mL; main effect, p = 0.05). Genotype tended to interact with maternal choline intake (p < 0.1) to influence newborn DHA status for PEMT rs4646343 and PEMT rs7946. These data support the need to consider variants in one-carbon metabolic genes in studies assessing DHA status and requirements during pregnancy.

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