Abstract

This administrative supplement is focused on adding targeted research questions related to Downs Syndrome (DS) across the Vanderbilt Kennedy Center?s (VKC) IDDRC, primarily enhancing Aim 3 of the Biostatistics and Bioinformatics Core, and also Aim 2 of the Clinical Translational Core. The proposed supplement focuses on Component 2 of NOT-OD-18-194 by proposing to conduct comprehensive molecular and phenotypic analysis in DS. Research activities will capitalize on Vanderbilt?s 20+ year mineable database of electronic medical records (named the Synthetic Derivative; SD) and BioVU (de-identified DNA samples that can be linked to data in the SD). SD/BioVU data allow for phenotypic and biological markers of DS to be examined, including longitudinally, in order to understand the sequela of disorders/conditions and/or biological markers associated with DS. While these are rich datasets, they are complex and require unique considerations. To this end, we have developed tools and approaches to leverage the depth of this data in order to study Autism Spectrum Disorder (ASD). In the supplement, we will apply these already developed tools and approaches to DS. Such data could be used, for example, in a predictive analytics framework to identify the best predictors of needing heart surgery. Also, we will capitalize on the BioVU DNA repository and the ongoing extensive efforts of the Vanderbilt Genetics Institute (VGI) to use a novel genetic approach to identify genetic risk factors for congenital heart disease in DS. The genotyping data developed from this will effort will also be useful for future studies of genetic risk factors for other co-morbid conditions in DS. The proposed work fits within the overarching IDDRC Aims to:
(Aim 1, Overview) build an innovative research infrastructure [with] new technological or other advances to the cores and provide essential services not otherwise available to IDDRC scientists and (Aim 2, Overview) to improve the health, education, and well-being of people with autism, learning disabilities, acquired disabilities, and genetic syndromes. More explicitly, though, it directly enhances the Biostatistics and Bioinformatics Core?s Aim 3, which focuses on developing electronic medical record (EMR) and genomic databases in a range of IDD conditions, including identifying specific variables of interest in the EMR; designing and programming optimal algorithms for identifying patients of interest from the SD; and, linking these data to existing patient DNA sequence or genotype data.
Aim 3 of the Biostatistics and Bioinformatics Core crosses with the Clinical and Translational Core?s Aim 2 goal of facilitating recruitment and data mining of longitudinal social, cognitive, and medical phenotypes in IDDs. Thus, the proposed activities enhance existing IDDRC aims, but rest squarely within the scope of them. The proposed work is targeted to be completed within a one-year timeframe, and the expected outcomes are to: (1) determine phenotypic associations with DS; (2) determine longitudinal predictors of outcomes; (3) determine how genetic variants within DS are related to these outcomes; and (4) increase VKC DS Registry and DSConnect registrants.

Public Health Relevance

This IDDRC administrative supplement application for Vanderbilt University's Intellectual and Developmental Disabilities Research Center (IDDRC), based in Vanderbilt's Kennedy Center (VKC), will use leverage existing electronic medical record information and biological samples to develop a deeper understanding of critical issues in Down Syndrome (DS) and provide and infrastructure for future analyses. Specifically, this work will: 1) identify unrecognized clinical features in DS and determine whether there are clinical features that differ between sexes and demographic groups; 2) develop predictive models based on EMR data for risk of clinical features or interventions in DS; 3) Identify genetic risk factors for congenital heart disease in DS. Finally, we will expand the prospective data collection in order to allow for future substantial and substantive DS research.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
3U54HD083211-05S1
Application #
9749464
Study Section
Program Officer
Parisi, Melissa
Project Start
2015-09-17
Project End
2020-05-31
Budget Start
2018-09-13
Budget End
2019-05-31
Support Year
5
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
DUNS #
079917897
City
Nashville
State
TN
Country
United States
Zip Code
37232

  Publications

Simon, David M; Wallace, Mark T (2018) Integration and Temporal Processing of Asynchronous Audiovisual Speech. J Cogn Neurosci 30:319-337
Baranek, Grace T; Woynaroski, Tiffany G; Nowell, Sallie et al. (2018) Cascading effects of attention disengagement and sensory seeking on social symptoms in a community sample of infants at-risk for a future diagnosis of autism spectrum disorder. Dev Cogn Neurosci 29:30-40
Burke, Meghan M; Waitz-Kudla, Sydney N; Rabideau, Carol et al. (2018) Pulling back the curtain: Issues in conducting an intervention study with transition-aged youth with autism spectrum disorder and their families. Autism :1362361317753016
Ding, Zhaohua; Huang, Yali; Bailey, Stephen K et al. (2018) Detection of synchronous brain activity in white matter tracts at rest and under functional loading. Proc Natl Acad Sci U S A 115:595-600
Harbison, Amy L; Woynaroski, Tiffany G; Tapp, Jon et al. (2018) A new measure of child vocal reciprocity in children with autism spectrum disorder. Autism Res 11:903-915
Aboud, Katherine S; Barquero, Laura A; Cutting, Laurie E (2018) Prefrontal mediation of the reading network predicts intervention response in dyslexia. Cortex 101:96-106
Choi, Dahye; Conture, Edward G; Tumanova, Victoria et al. (2018) Young children's family history of stuttering and their articulation, language and attentional abilities: An exploratory study. J Commun Disord 71:22-36
Kim, Young-Suk Grace; Gatlin, Brandy; Al Otaiba, Stephanie et al. (2018) Theorization and an Empirical Investigation of the Component-Based and Developmental Text Writing Fluency Construct. J Learn Disabil 51:320-335
Bettis, Alexandra H; Forehand, Rex; Sterba, Sonya K et al. (2018) Anxiety and Depression in Children of Depressed Parents: Dynamics of Change in a Preventive Intervention. J Clin Child Adolesc Psychol 47:581-594
Mi, Deborah J; Dixit, Shilpy; Warner, Timothy A et al. (2018) Altered glutamate clearance in ascorbate deficient mice increases seizure susceptibility and contributes to cognitive impairment in APP/PSEN1 mice. Neurobiol Aging 71:241-254

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