Abstract

The Clinical Core of the UC Davis Alzheimer's Disease Center (UCD ADC) seeks to facilitate research on Alzheimer's disease in Northern California by creating for investigators a centralized source of carefully evaluated and well characterized dementia patients and normal controls and maintaining a database of clinical and neuropathological findings on these subjects. The UCD ADC has a large and diverse catchment area, encompassing the major cities and suburban areas of San Francisco, San Jose, Oakland, and Sacramento, large portions of the agricultural Central Valley, and rural areas to the east and north. Patients are referred from an extensive network of UC Davis clinics and facilities to 4 ADC performance sites; 2 main clinics (Berkeley and Sacramento) and 2 satellite clinics (Oakland and Yolo County). The Clinical Core provides the resources and personnel to combine these clinical dementia evaluation facilities into an integrated program with a shared research mission. The major functions of the Core are: 1) to create an ethnically diverse subject pool consisting of carefully diagnosed and well characterized dementia patients and normal controls, 2) to collect comprehensive and standardized clinical data on these subjects, 3) to create and manage a central database of diagnostic, clinical, and neuropathological findings, 4) to provide longitudinal follow-up, 5) to support research by identifying and recruiting patients and controls for specific studies, and 6) to operate satellite clinics to facilitate access of minority and under-served populations to Alzheimer's disease research. The Core recruits and evaluates demographically matched control subjects using the same protocols and methods as for patients and devotes considerable attention to issues of cross-site and inter-rater reliability, and to the development of innovative methods for quantitating clinical data. Finally, the Core facilitates autopsy for patients of research interest. In this renewal the Clinical Core proposes evolutionary modifications of the methods it employed in its first funding cycle. The Core will evaluate approximately 300 new patients and 100 new controls per year obtaining standardized histories, neurological exams, neuroimaging, laboratory, neuropsychological, behavioral and psychiatric data on all. It will maintain its longitudinal cohort of approximately 300 patients who are high quality research subjects and create a comparable longitudinal follow-up cohort of 200 control subjects who have consented to autopsy. The Core's two satellite clinics have evolved effective outreach methods which have resulted in substantial numbers of ethnic minority patients; the Core will build upon this clinical base to achieve an ethnically diverse and balanced research and autopsy sample. Data from all subjects will be entered to an extensive database and the Core will help enlist these subjects in individual research projects, track research participation, and help obtain autopsy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Center Core Grants (P30)
Project #
3P30AG010129-09S1
Application #
6216993
Study Section
Project Start
1999-08-15
Project End
2000-06-30
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
9
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of California Davis
Department
Type
DUNS #
094878337
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Hanfelt, John J; Peng, Limin; Goldstein, Felicia C et al. (2018) Latent classes of mild cognitive impairment are associated with clinical outcomes and neuropathology: Analysis of data from the National Alzheimer's Coordinating Center. Neurobiol Dis 117:62-71
Ting, Simon Kang Seng; Foo, Heidi; Chia, Pei Shi et al. (2018) Dyslexic Characteristics of Chinese-Speaking Semantic Variant of Primary Progressive Aphasia. J Neuropsychiatry Clin Neurosci 30:31-37
Jena, Prasant Kumar; Sheng, Lili; Di Lucente, Jacopo et al. (2018) Dysregulated bile acid synthesis and dysbiosis are implicated in Western diet-induced systemic inflammation, microglial activation, and reduced neuroplasticity. FASEB J 32:2866-2877
Burke, Shanna L; Hu, Tianyan; Fava, Nicole M et al. (2018) Sex differences in the development of mild cognitive impairment and probable Alzheimer's disease as predicted by hippocampal volume or white matter hyperintensities. J Women Aging :1-25
Maezawa, Izumi; Nguyen, Hai M; Di Lucente, Jacopo et al. (2018) Kv1.3 inhibition as a potential microglia-targeted therapy for Alzheimer's disease: preclinical proof of concept. Brain 141:596-612
Meyer, Oanh L; Liu, Xiaoyan Lucia; Tancredi, Daniel et al. (2018) Acculturation level and caregiver outcomes from a randomized intervention trial to enhance caregivers' health: evidence from REACH II. Aging Ment Health 22:730-737
Fletcher, Evan; Gavett, Brandon; Harvey, Danielle et al. (2018) Brain volume change and cognitive trajectories in aging. Neuropsychology 32:436-449
Wang, Qi; Guo, Lei; Thompson, Paul M et al. (2018) The Added Value of Diffusion-Weighted MRI-Derived Structural Connectome in Evaluating Mild Cognitive Impairment: A Multi-Cohort Validation1. J Alzheimers Dis 64:149-169
Dadar, Mahsa; Maranzano, Josefina; Ducharme, Simon et al. (2018) Validation of T1w-based segmentations of white matter hyperintensity volumes in large-scale datasets of aging. Hum Brain Mapp 39:1093-1107
Wong, Jonathan M; Gray, John A (2018) Long-Term Depression Is Independent of GluN2 Subunit Composition. J Neurosci 38:4462-4470

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