Pregnancy Clinical Trial
Official title:
Investigation Into the Influence of Genetic Variation on Folate, Cobalamin and Related Metabolites
This study will examine how the body metabolizes micronutrients, such vitamins, during
pregnancy and how genetic make-up influences their metabolism. Vitamin B12 and folate levels
in pregnancy have been linked to birth defects, such as neural tube defects, orofacial
clefts, and congenital heart disease. Other micronutrient levels may be related to other
birth defects or pregnancy complications. This study will characterize the patterns of
micronutrient status during pregnancy and compare it with genetic variants and biochemical
parameters. Information about the relationship between genes and vitamin metabolism may help
doctors advise women about their nutritional requirements during pregnancy to protect their
health and the health of their babies.
This study is a collaboration between NIH and Trinity College in Dublin, Ireland. Women of
Irish origin 18 years of age or older who are receiving prenatal care at the Coombe Women's
Hospital in Dublin may be enrolled. Fathers also may participate.
Upon entering the study, female participants complete a questionnaire relating to their food
and vitamin intake, alcohol consumption, smoking behavior, and use of medications, and
provide a blood sample. Additional blood samples are collected during routine clinic visits
at about 24 and 34 weeks of pregnancy, and again at delivery and from 6 weeks to 2 months
after the baby's birth. Permission will be requested to obtain a blood sample from the
umbilical cord at birth after it has been removed from the baby.
Fathers of the babies are also asked to answer a short questionnaire and to provide a DNA
sample for genetic studies. To collect the DNA, sterile cotton swabs are rubbed around the
inside of the mouth to obtain cheek cells from which the DNA is extracted.
A number of genetic polymorphisms influence human folate, vitamin B12 and related micronutrient levels. Vitamin B12 and folate levels in pregnancy have been linked to birth defects including neural tube defects, orofacial clefts, and congenital heart disease. Additionally, related analytes, such as homocysteine, may be related to birth defects and pregnancy complications. The behavior of maternal serum micronutrients and related analytes throughout human pregnancy is not well described. In this study, we aim to characterize the patterns of micronutrient status during pregnancy. We plan to perform biochemical analyses on serial blood samples collected from 500 pregnant women at five intervals spanning early pregnancy and the post partum period. We will also characterize neonatal micronutrient status using a specimen of umbilical cord blood. These blood specimens, as well as buccal swab specimens collected from the fathers, will also be evaluated to measure the influence of genetic variants on metabolite levels. The major outcomes measured will be longitudinal maternal micronutrient levels and aggregate alleel frequencies among family triads. Comparisons will be made between the presence of genetic variants, biochemical parameters, and clinical phenotype. At a later date we also plan to study the same metabolic and genetic parameters in a large cohort of healthy individuals. Characterizing these biochemical and genetic variants should provide insight into the metabolic processes of normal and complicated pregnancies. ;
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