Abstract

Down syndrome (DS) or trisomy for chromosome 21, is a major cause of mental retardation and congenital heart disease, that affects more than 400,000 individuals in the USA. In addition, people with DS have defects in memory, language and neuroanatomy. The ultimate goal of this proposal is to elucidate the genes, neuroanatomy and neurocircuitry linked to the neurocognitive defects of DS. Recent advances in human genome sequencing provide a complete list of chromosome 21 genes, but until recently (Korbel, 2009), there were no genes linked to any specific feature and no successful treatment for the cognitive deficits. Treatment of DS has been hindered by lack of human models for narrowing the genes responsible for cognitive features, the need for high resolution neuroimaging of the brain defects in DS and the need for cognitive tests focused on DS deficits. To address these gaps, we propose an innovative multidisciplinary approach integrating neuroimaging, cognitive testing and genetics. In DS as in genetics, rare events can illuminate common processes. Rare individuals have DS caused by duplication of only parts of chromosome 21 and provide a unique opportunity to link the defects of brain development and function with the genes responsible. The PI of this proposal has generated the largest cohort in existence, consisting of 45 persons, of whom 30 are alive, in the USA, 27 aneuploid only for 21. Recently, these rare cases were used to map specific gene subsets in DS for congenital malformations but little was known about the brain or cognition. Further, a unique and rare set of identical twins discordant for DS, has been identified and studied. To characterize these cohorts, a unique team of scientists has been created, with expertise in partial trisomy 21 (Korenberg), neurocognitive testing targeted to DS (Nadel, Yurgelun-Todd), Magnetic Resonance Imaging and Diffusion tensor imaging (Yurgelun- Todd, Gerig), NMR Spectroscopy (Renshaw) and genome organization (Korenberg). This team will integrate high resolution imaging of full and rare partial trisomy 21 to establish the regional neuroanatomy and neurocircuitry of DS and to link these to subsets of chromosome 21 genes. We will test three levels of hypotheses, first to define in DS vs normals, distinct volumetric and circuit brain structures and defects of cognitive function, including language and memory;second, to link within DS, neural substrates with cognitive features and third, by using each rare partial trisomy, to begin to parse gene subsets for DS neural and cognitive features. Further, we will test in DS, whether the glutamatergic or, as in mouse, the GABAergic neurotransmitter systems are disturbed in vivo. We propose two aims: 1) to characterize 60 normal and 60 full trisomy 21 individuals with cognitive testing, high resolution MRI, DTI and MRS, 2) to characterize the rare DS cohort with partial trisomy 21 and the unique set of identical twins discordant for DS as in aim 1. The results of these studies will provide unprecedented knowledge of the defects of brain development and function in DS, GABAergic and glutamatergic pathways, and the relationship of both to genes duplicated. These results will help to elucidate the neurobiology of DS and to develop novel treatments for DS and other intellectual disabilities.

Public Health Relevance

The children of our nation are its most precious resource and those with developmental disabilities pose one of the most significant challenges our nation faces not only because 4.5 million are afflicted with these debilitating disorders but in addition, these individuals hold the key to understanding the biologic underpinnings of brain diseases, including Alzheimer's disease (5.3 million affected, $148 billion cost/year in the USA) and intellectual disability (>1.5 million affected, $51.2 billion cost/year in the USA). No where is this challenge more clearly defined than for Down syndrome, the most common genetic cause of mental disability and of Alzheimer's disease. Critically, due to the increased risk, DS also promises to provide insight into the common conditions relating to congenital heart and gut malformations and leukemia, and in contrast, the promise of clues to novel treatments for solid tumors and atherosclerosis, diseases for which they have decreased risk. DS affects the families of more than 400,000 in the USA alone, with a societal cost of more than $800 million each year and $4.5 billion lifetime direct and indirect costs per cohort at a 2% discount rate. Recently powerful new advances in human brain imaging and genetics have revolutionized medical neurosciences, providing the opportunity for novel techniques to unlock the secrets linking genes to the brain in Down syndrome. We now propose to apply a cross-disciplinary approach including genetics, neuroanatomy (MRI), neural circuitry (DTI), neurotransmitter (MRS) and neurocognitive features to the study of Down syndrome. Findings from these studies will provide new insights into the genetics and development of the human brain, and into treatment strategies including new drug targets for prevention, recovery and ultimately cure of mental disability.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD067731-02
Application #
8313895
Study Section
Special Emphasis Panel (ZRG1-BBBP-N (03))
Program Officer
Oster-Granite, Mary Lou
Project Start
2011-08-10
Project End
2016-05-31
Budget Start
2012-06-01
Budget End
2013-05-31
Support Year
2
Fiscal Year
2012
Total Cost
$581,931
Indirect Cost
$192,679

  Institution

Name
University of Utah
Department
Pediatrics
Type
Schools of Medicine
DUNS #
009095365
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Hunsaker, Michael R; Smith, Genevieve K; Kesner, Raymond P (2017) Adaptation of the Arizona Cognitive Task Battery for use with the Ts65Dn mouse model (Mus musculus) of Down syndrome. J Comp Psychol 131:189-206
Elhabian, Shireen; Vachet, Clement; Piven, Joseph et al. (2016) Compressive Sensing Based Q-Space Resampling for Handling Fast Bulk Motion in Hardi Acquisitions. Proc IEEE Int Symp Biomed Imaging 2016:907-910
Anderson, Jeffrey S; Treiman, Scott M; Ferguson, Michael A et al. (2015) Violence: heightened brain attentional network response is selectively muted in Down syndrome. J Neurodev Disord 7:15
Durrleman, Stanley; Prastawa, Marcel; Charon, Nicolas et al. (2014) Morphometry of anatomical shape complexes with dense deformations and sparse parameters. Neuroimage 101:35-49
Smith, Genevieve K; Kesner, Raymond P; Korenberg, Julie R (2014) Dentate gyrus mediates cognitive function in the Ts65Dn/DnJ mouse model of Down syndrome. Hippocampus 24:354-62
Anderson, Jeffrey S; Nielsen, Jared A; Ferguson, Michael A et al. (2013) Abnormal brain synchrony in Down Syndrome. Neuroimage Clin 2:703-15
Sadeghi, Neda; Prastawa, Marcel; Fletcher, P Thomas et al. (2013) Regional characterization of longitudinal DT-MRI to study white matter maturation of the early developing brain. Neuroimage 68:236-47
Durrleman, S; Pennec, X; Trouvé, A et al. (2013) Toward a comprehensive framework for the spatiotemporal statistical analysis of longitudinal shape data. Int J Comput Vis 103:22-59
Sadeghi, Neda; Prastawa, Marcel; Fletcher, P Thomas et al. (2013) MULTIVARIATE MODELING OF LONGITUDINAL MRI IN EARLY BRAIN DEVELOPMENT WITH CONFIDENCE MEASURES. Proc IEEE Int Symp Biomed Imaging :1400-1403
Sharma, Anuja; Durrleman, Stanley; Gilmore, John H et al. (2013) LONGITUDINAL GROWTH MODELING OF DISCRETE-TIME FUNCTIONS WITH APPLICATION TO DTI TRACT EVOLUTION IN EARLY NEURODEVELOPMENT. Proc IEEE Int Symp Biomed Imaging 2012:1945-1400

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