Metabolic Syndrome Clinical Trial
Official title:
Identifying Biomarkers and Cardiovascular Risk Factors in Childhood Metabolic Syndrome
Metabolic syndrome (MetS) is highly prevalent all over the world. MetS is largely
under-diagnosed in children and adolescents. Obesity and hypertension are two important
requirements for criteria of MetS. With early detection and early intervention of MetS in
children and adolescents will enable better care to reduce the heavy burden of health care
all over the world.
Investigators intend to recruit 150 children and adolescents age 6 to 18 yr with
overweight/obesity or prehypertension/hypertension and 50 normal age-matched controls to
reach the following research goals:
1) To identify biomarkers as risk factors; 2) To characterize that impact of vascular
assessment in preMetS children; and 3) To examine the relationship among biomarkers, vascular
assessment parameters, and metabolic phenotypes.
Metabolic syndrome (MetS) is highly prevalent all over the world, including Taiwan. So far,
there is still no standard definition of MetS for use in pediatric population. Thus MetS is
largely under-diagnosed in children and adolescents. Obesity and hypertension are two
important requirements for criteria of MetS. With early detection and early intervention of
MetS in children and adolescents will enable better care to reduce the heavy burden of health
care all over the world.
MetS might originate from early life, namely developmental programming. Cardiovascular
disease (CVD) is the most common comorbidity of MetS. Therefore identification of biomarkers
for detecting children with high-risk to develop CVD and MetS progression is our priority.
Investigators' previous studies identified some biomarkers from a variety of programming
models, including asymmetric dimethylarginine (ADMA, a nitric oxide synthase inhibitor),
β-trace protein (BTP, also known as lipocalin-type prostaglandin D synthase), and
adiponectin. Thus, in the current study, ADMA profile, BTP, and adiponectin will be studied
in children and adolescents with pre-MetS to explore their role as biomarkers to predict MetS
and CVD progression.
In childhood, assessment of CVD relies on endothelial function and arterial stiffness, as CV
events are extremely rare. Thus, in this study investigators intend to perform a global
vascular assessment (to determine endothelial function and arterial stiffness) in children
with pre-MetS including 24hr ABPM, measure of pulse wave velocity (PWV) and ambulatory
arterial stiffness index (AASI) to detect arterial stiffness, detection of flow mediated
dilatation (FMD), and biomarkers. Investigators also intend to examine the correlation
between biomarkers and these measured vascular parameters in children with preMetS.
Therefore, investigators will recruit 150 children and adolescents age 6 to 18 yr with
overweight/obesity or prehypertension/hypertension and 50 normal age-matched controls to
reach the following research goals:
1) To identify biomarkers as risk factors; 2) To characterize that impact of vascular
assessment in preMetS children; and 3) To examine the relationship among biomarkers, vascular
assessment parameters, and metabolic phenotypes.
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