Gestational Diabetes Clinical Trial
Official title:
Possible Epigenetic Changes in Offspring of Women With Pregestational and Gestational Diabetes: Molecular Studies of the Placenta and Cord Blood and Possible Correlation to Postnatal Development.
Pregestational diabetes (PGD) during pregnancy may be associated with an increased rate of
spontaneous abortions, intrauterine death and congenital anomalies among the offspring.
Although the prevalence of congenital anomalies among the offspring of diabetic mothers is
reduced as a result of the improvement of the glycemic control in the early pregnancy, the
rate of congenital anomalies is increased and there seems to be an increased rate of
neurodevelopmental disorders including some fine and gross motor deficits as well as
increased rate of inattention and/or hyperactivity. In gestational diabetes, that develops
in the second half of pregnancy (past the period of major organogenesis), there seems to be
no increase in the rate of major congenital anomalies but there are some developmental
disorders in the offspring.
The exposure of the developing embryo and fetus to diabetic environment (i.e. hyperglycemia,
hyperketonemia ext), is known to cause increased oxidative stress and significant changes in
gene expression as observed in several experimental diabetic models. We hypothesize that
diabetic environment may also cause long lasting epigenetic changes. It is therefore our
purpose to evaluate these possible epigenetic changes and correlate their presence with the
degree and time of onset of diabetes, (i.e. whether from the beginning as in PGD or in the
second half of pregnancy as in GD), the degree of oxidative stress and with the
neurodevelopmental outcome of the offspring. Diabetic pregnancies will be compared to a
similar number of normal pregnancies in all parameters studied.
n/a
Observational Model: Case Control, Time Perspective: Prospective
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