Obesity Clinical Trial
To determine whether maternal undernutrition in pregnancy is associated with differences between siblings for cardiovascular risk factors in adulthood.
BACKGROUND:
A variety of studies have reported associations between birth weight and other proxy
measures of fetal nutrition and chronic disease risk in adulthood, particularly "metabolic
diseases" such as type 2 diabetes and cardiovascular disease (CVD). These findings have led
to the theory of "fetal programming" of adult chronic disease. This theory is highly
provocative because it suggests that the prevention of many chronic diseases should start
with the improvement of materno-fetal nutrition. A mechanism for fetal programming of adult
chronic disease risk, however, has not been identified. In addition, most epidemiological
studies have been ecological and retrospective, with poor identification of exposure dose
and timing, and control of confounders.
DESIGN NARRATIVE:
The cohort study determines whether famine exposure during the first, second, or third
trimesters of gestation is associated with differences between sibs for CVD risk factors in
adulthood, specifically centralized obesity, insulin resistance, increased blood pressures,
dyslipidemia, and diagnosed type 2 diabetes. Using the data collected, the investigators
propose to: (1) evaluate the key assumption that maternal undernutrition during pregnancy
results in fetal programming of CVD risk factors; (2) better identify the critical period
during gestation in which this may occur; and, (3) determine the strength of the
associations with chronic disease risk factors in adulthood.
The study will utilize an innovative sib-pair design in which cases, or "probands," exposed
to fetal undernutrition during the Dutch Famine during 1944-45, will be matched to same-sex
full siblings who were born in different years and not exposed. The timing of births within
the famine period will allow the investigators to classify proband exposure approximately by
trimester of gestation. Thus, compared to most previous studies, they will be better able to
identify the "critical period" - early, mid, or late gestation - during which fetal
programming effects are most likely to occur. In addition, the investigators will randomly
select a sample of unexposed probands with birth dates in 1943 or 1947, immediately before
and after the famine, and matched siblings. All exposed and unexposed probands will be
ascertained from the prenatal and delivery records of three hospitals in the Western
Netherlands where the famine was most intense. These records include information on maternal
and family medical history, socioeconomic status, pregnancy characteristics (blood pressure,
weight gain, etc.), and birth outcomes, including anthropometry and gestational age.
Siblings will be identified using national Population Registers (Bevolkings registers), and
hospital prenatal and delivery records will be obtained.
In addition to collecting information from perinatal hospital and registry records, all
subjects will undergo a home interview and clinical examination. The interview will collect
information on sociodemographic characteristics, economic status, health history, including
obstetric history, current health and medical treatment, and health behaviors, including
physical activity. The clinical examine will include a fasting blood draw for lipid,
glucose, and insulin concentrations, and a glucose tolerance test with additional blood
draws at 30 and 120 minutes post-glucose load. Blood will also be stored for future DNA
isolation and assay of genetic polymorphisms that could influence associations among the
study variables. Anthropometry will include height, weight, waist circumference, and
abdominal sagital diameter. A food frequency questionnaire will also be administered during
either the interview or examination phase.
An innovative part of the study will be measurements of hand morphology: specifically,
fingertip ridge-count differences and digit-lengths. These characteristics are established
by the 19th week of gestation and are fixed thereafter throughout the lifetime. There is
some evidence that the development of these characteristics prior to 19 weeks of gestation
may be influenced by environmental factors, including materno-fetal nutrition. The
investigators will test the hypothesis that these finger and hand characteristics are
markers of undernutrition during the first half of pregnancy and predict other adult CVD
risk factors.
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