Neurodevelopmental Disorders Clinical Trial
Official title:
Early Biomarkers of Neurodevelopment in Offspring of Diabetic Mothers (GD-BRAIN)
The prospective multicenter study GD-Brain provides a better knowledge on the basis of
neurological impairment in children born to mothers with gestational diabetes (GDM). GDM
modifies placental structure and affect materno-fetal nutrient transfer. Docosahexaenoic
acid (DHA) play an important role on neurodevelopment, and it is reduced in venous cord
blood of newborns born to GDM. In previous studies, we have already demonstrated impaired
DHA fetal levels not only using label fatty acids with stable isotopes administrated to
pregnant women, but also in observational studies in GDM as the prevention of obesity study
(PREOBE study) in Granada and other similar study in Murcia. The impaired cord DHA levels
were associated to disturbed neurodevelopment in these children during the first year of
life. However, it is uncertain the mechanisms underlying this impaired materno-fetal DHA
transfer and implications for later life.
The recent publication in Nature Journal of a selective transmembrane carrier for DHA in
brain named "major facilitator superfamily domain 2a" (MFSD2a) open new expectations. We
detected disturbed MFSD2a levels in placentas from GDM which could be due to structural
problems in this organ; inflammation, oxidation and metabolic changes related to diabetes
might affect MFSD2a activity. Moreover, it is difficult to know whether disturbed MFSD2a
levels in placenta may also indicate altered levels of this carrier in the brain from
children born to GDM mothers, which could contribute to neurodevelopment impairment in these
subjects. Recent studies also indicate that obesity alters the biosynthesis of eicosanoids
derived from DHA, with a decrease of protectins and resolvin of D-series, which have
powerful anti-inflammatory properties.
The main aim of this study is to analyse potential differences on neurodevelopment, and
brain structure and functioning, in children 8 years old born to GDM respect to those born
to healthy normoweight mothers, as well as to identify early biomarkers consistently related
to neurodevelopment from early stages of life.
We will contact to participants from the PREOBE study and Murcia's cohorts study to get
involved a total of 174 children at 8 years of age. The results from neurodevelopment
evaluation by neuropsychological testing, neurological functions rhythms and neuroimaging
(fMRI and DTI) at 8 years old will be associated to clinical and metabolic data recorded
during pregnancy.
As secondary aim, we would discern whether the decrease on DHA levels in offspring of GDM at
birth is associated to disturbed neurodevelopment at 8 years old.
The impact of maternal diabetes on placental MFSD2a and children's resolvin and protectins
derived from DHA will be measured in urine samples at 8 years old.
Gut microbiota composition and function will be also studied to detect its role in the
potential disturbances regarding the production of anti-inflammatory mediators.
A part from the clinical study, we will perform an intervention trial using animal models.
Gestational rats with diabetes and control rats will be treated with antioxidants and
adipoRon in order to delay neuro-degeneration in these animals because of the diabetes, as
well as their influence on MFSD2a levels in placenta and brain. All these studies may
provide to the industry of valuable information to improve nutritional supplements during
gestation or infancy to avoid potential delay of cognitive functions in offspring of
diabetic mothers.
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