Abstract

The purpose of the present study is to investigate relationships between novel neuroimaging markers based on DTI fiber tracking models, genetic polymorphisms of vascular disease and inflammation, and age-related cognitive decline in healthy individuals. Recent studies, including data from our lab, indicate that the integrity of the subcortical white matter as measured by diffusion tensor imaging (DTI) and subcortical hyperintensities on structural MRI are important correlates of age-related cognitive differences. Cortical brain volume changes also account for some variance in cognitive function among the elderly, however our data suggest that alterations in the subcortical white matter more strongly correlate with cognitive status. In addition, studies have demonstrated that white matter alterations in the elderly are heritable, implicating the role of genetic factors in the development of mild ischemic changes and associated inflammation. In this revised application we provide compelling new pilot data demonstrating the role of genetic polymorphisms for vascular injury on both imaging and cognitive indices. We also provide new data from our recent work demonstrating the sensitivity of our novel DTI metrics based on quantified fiber tracking models to explain variance in cognitive aging. These novel metrics allow us to examine the impact of changes in quantified fiber lengths on cognitive function. In the present study we will extend these preliminary studies and examine relationships between DTI and structural MRI, genetic polymorphisms associated with microvascular disease (angiotensinogen, paroxonase) and related CMS inflammation (C-reactive protein, IL- 6, TNF-a), and cognitive status in the healthy elderly. The study will capitalize on an existing database containing genetic and neurocognitive data on more than 1,000 individuals stratified in five groups from age 31-80 (n = 200/group). Neuroimaging data is currently available for 200 of these individuals and we will recruit an additional 120 individuals between the ages of 51-80 to supplement the older age spectrum and obtain novel fiber tracking maps from the DTI data. Newly recruited individuals will be followed longitudinally to examine the evolution and progression of white matter and cognitive abnormalities in the context of genetic risk factors. Group comparisons and latent variable modeling will be conducted to examine relationships between the neuroimaging indices, genetic polymorphisms, and differences in cognitive function in older healthy adults. The present study will be the first to integrate these approaches to examine a model of age-related cognitive decline implicating the subcortical white matter. The results will significantly inform our understanding of cognitive aging. ? ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS052470-01A2
Application #
7262790
Study Section
Clinical Neuroscience and Disease Study Section (CND)
Program Officer
Babcock, Debra J
Project Start
2007-07-01
Project End
2012-06-30
Budget Start
2007-07-01
Budget End
2008-06-30
Support Year
1
Fiscal Year
2007
Total Cost
$576,718
Indirect Cost

  Institution

Name
University of Missouri-St. Louis
Department
Psychology
Type
Schools of Arts and Sciences
DUNS #
804883825
City
Saint Louis
State
MO
Country
United States
Zip Code
63121

  Publications

Cabeen, Ryan P; Bastin, Mark E; Laidlaw, David H (2017) A Comparative evaluation of voxel-based spatial mapping in diffusion tensor imaging. Neuroimage 146:100-112
Salminen, Lauren E; Schofield, Peter R; Pierce, Kerrie D et al. (2017) Vulnerability of white matter tracts and cognition to the SOD2 polymorphism: A preliminary study of antioxidant defense genes in brain aging. Behav Brain Res 329:111-119
Salminen, Lauren E; Schofield, Peter R; Pierce, Kerrie D et al. (2016) Neuromarkers of the common angiotensinogen polymorphism in healthy older adults: A comprehensive assessment of white matter integrity and cognition. Behav Brain Res 296:85-93
Salminen, Lauren E; Conturo, Thomas E; Bolzenius, Jacob D et al. (2016) REDUCING CSF PARTIAL VOLUME EFFECTS TO ENHANCE DIFFUSION TENSOR IMAGING METRICS OF BRAIN MICROSTRUCTURE. Technol Innov 18:5-20
Heaps-Woodruff, J M; Wright, P W; Ances, B M et al. (2016) The impact of human immune deficiency virus and hepatitis C coinfection on white matter microstructural integrity. J Neurovirol 22:389-99
Baker, Laurie M; Cabeen, Ryan P; Cooley, Sarah et al. (2016) APPLICATION OF A NOVEL QUANTITATIVE TRACTOGRAPHY-BASED ANALYSIS OF DIFFUSION TENSOR IMAGING TO EXAMINE FIBER BUNDLE LENGTH IN HUMAN CEREBRAL WHITE MATTER. Technol Innov 18:21-29
Salminen, Lauren E; Conturo, Thomas E; Laidlaw, David H et al. (2016) Regional age differences in gray matter diffusivity among healthy older adults. Brain Imaging Behav 10:203-11
Cabeen, Ryan P; Bastin, Mark E; Laidlaw, David H (2016) Kernel regression estimation of fiber orientation mixtures in diffusion MRI. Neuroimage 127:158-172
Luo, X; Gee, S; Sohal, V et al. (2016) A point-process response model for spike trains from single neurons in neural circuits under optogenetic stimulation. Stat Med 35:455-74
Behrman-Lay, Ashley M; Usher, Christina; Conturo, Thomas E et al. (2015) Fiber bundle length and cognition: a length-based tractography MRI study. Brain Imaging Behav 9:765-75

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