Physiological Abnormalities Associated with Down Syndrome

University of Arkansas

Status

Withdrawn

Conditions

Down Syndrome

Study type

Observational

Funder types

Other

Identifiers

NCT03087500

206522

Details and patient eligibility

About

The overall goal of this study is to evaluate biomarkers of oxidative stress, mitochondrial function, and DNA methylation (epigenetics) in order to determine the extent to which these biomarkers are related to cognitive, behavioral and adaptive function in Down Syndrome. The inter-relationship between measurable biomarkers and functional/cognitive abilities will move beyond genetics to provide unprecedented new knowledge and a broader understanding of the underlying pathophysiology and abnormal gene expression induced by trisomy 21.

Full description

The Investigators preliminary evidence indicates that people with DS have metabolic biomarkers associated with oxidative stress (GSH/GSSG) and reduced methylation capacity (SAM/SAH) as well as abnormal DNA methylation (epigenetics). The investigative team hypothesize that these abnormal metabolic processes contribute to abnormalities in behavior and development associated with trisomy 21; this connection has never been investigated. Confirming and expanding on the preliminary data would provide new understanding of the biological and functional etiology of the behavioral and developmental delays associated with Trisomy 21. Further, establishing the underlying relationship between metabolic abnormalities and behavioral/cognitive function over the age spectrum can provide strong support for the design of future treatments of individuals with DS aimed at improving their behavior and development. In addition, these biomarkers may also prove to be predictive biomarkers for the risk of developing ASD like behaviors or Alzheimer's disease in this population. Finally, examining the modulating role of diet in the severity of biological abnormalities will provide new information for lifestyle guidance to improve biomarkers and potentially minimize the medical co-morbidities associated with trisomy 21.

Sex

All

Ages

3 to 50 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Participant or guardian ability to consent/assent and willing to comply with protocol requirements

Exclusion criteria

Trisomy translocation or mosaics.
Untreated hypothyroidism
Known history of liver disease, renal disease, Hepatitis B or C or HIV
Recent infection with fever or requiring hospitalization within past 30 days.
Any medical condition, use of medications, nutrient or herbal supplements that would interfere with the study results as determined by the PI
Chemotherapy
Recent surgery (within 2 months)
Untreated Epilepsy
Any chronic medical/behavioral condition and/or treatments that may interfere with study related outcomes, as determined by PI
Dementia
History of a significant adverse reaction to a prior blood draw
Any other historical event/information that may, in the opinion of the PI, be a reason to exclude the child from participation.

Trial design

0 participants in 2 patient groups

Down Syndrome (DS)

Description:

120 clinically confirmed full trisomy 21, age 3-50 years of both sexes will be recruited as the target study population. Half of the individuals (n=60) will be children (3-17 years of age) while half (n=60) will be adults (18-50 years of age)

Typically Developing Controls

Description:

60 typically developing individuals age 3-50, age and gender matched to at least one participant with DS. Half of the controls (n=30) will be age and gender match to children with DS and half (n=30) will be age and gender matched to adults with DS.

Trial contacts and locations

Data sourced from clinicaltrials.gov

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