Abstract

The role of the tau protein in neurological diseases is an important open question, given that it has been demonstrated as a central driver of neurodegeneration. Though tau's pathogenic mechanisms are still unclear, variants in the MAPT gene, encoding for tau, have been identified as causal in some tauopathies, and the H1 haplotype at the 17q21.31 locus (containing MAPT) has been strongly linked to risk for progressive supranuclear palsy (PSP), which is pathologically the purest tauopathy. However, the use of traditional techniques such as genome-wide association studies (GWAS) has stalled in advancing this field due to limited scope of data and lack of statistical power. Meanwhile, emerging technologies such as next-generation sequencing allow the generation of richer sets of genetic, epigenetic, and gene expression data. Using such methods, we have discovered potential factors on the molecular level that contribute to certain tauopathies in human blood cells. In this proposal we aim to expand and leverage these diverse datasets in an integrative fashion to overcome the limitations of traditional statistical approaches and provide mechanistic insight into the pathogenicity of tau protein. First, we will extend our analysis of H1 haplotype differential gene expression and epigenetic changes from blood cells to human brain regions, using RNA-seq of cells from multiple brain regions of normal subjects. These findings will be confirmed and validated for involvement in disease using real-time PCR experiments in brains from PSP cases. Second, we will detect novel alleles outside of the tau locus that modify risk for PSP. Besides the fact that our cohort is the only dataset of PSP patients for which whole-genome sequencing is available, we additionally have data regarding DNA methylation and gene expression from the same subjects. Integrative analyses of such data using methods of rare variant association, clustering, and causality analysis will be able to discover effects which were previously undetectable, and provide biological and functional context. Third, we will use genomic editing by transcription activator-like effector nucleases (TALENs) to introduce candidate mutations into cell lines. This experiment will thereby generate cell models of tauopathy, experimentally validate mechanistic findings, and provide strong causal evidence. By performing this work, we will discover genetic factors that contribute to tauopathies and the mechanisms by which they operate, findings of diagnostic and therapeutic significance.

Public Health Relevance

The tauopathies encompass a group of neurodegenerative disease, including Alzheimer's disease (AD), Frontotemporal Dementia (FTD), Progressive Supranuclear Palsy (PSP), and others, and are collectively responsible for the majority of dementia cases. We propose an integrative genomics study of patients affected by such diseases to detect genes and mutations that are involved in tau pathogenicity. Elucidating this genetic contribution to tauopathies may ultimately yield 1) richer understanding of disease mechanisms;2) improved genetic diagnosis;and 3) drug targets with potential therapeutic value.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Predoctoral Individual National Research Service Award (F31)
Project #
5F31NS084556-02
Application #
8718814
Study Section
Neurological Sciences Training Initial Review Group (NST)
Program Officer
Sieber, Beth-Anne
Project Start
2013-08-01
Project End
2017-07-31
Budget Start
2014-08-01
Budget End
2015-07-31
Support Year
2
Fiscal Year
2014
Total Cost
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
Overall Medical
DUNS #
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Chen, Jason A; Fears, Scott C; Jasinska, Anna J et al. (2018) Neurodegenerative disease biomarkers A?1-40, A?1-42, tau, and p-tau181 in the vervet monkey cerebrospinal fluid: Relation to normal aging, genetic influences, and cerebral amyloid angiopathy. Brain Behav 8:e00903
Chen, Jason A; Chen, Zhongbo; Won, Hyejung et al. (2018) Joint genome-wide association study of progressive supranuclear palsy identifies novel susceptibility loci and genetic correlation to neurodegenerative diseases. Mol Neurodegener 13:41
Lopez, Ana; Lee, Suzee E; Wojta, Kevin et al. (2017) A152T tau allele causes neurodegeneration that can be ameliorated in a zebrafish model by autophagy induction. Brain 140:1128-1146
Chen, Jason; Yu, Jin-Tai; Wojta, Kevin et al. (2017) Genome-wide association study identifies MAPT locus influencing human plasma tau levels. Neurology 88:669-676
Chen, Jason A; Wang, Qing; Davis-Turak, Jeremy et al. (2015) A multiancestral genome-wide exome array study of Alzheimer disease, frontotemporal dementia, and progressive supranuclear palsy. JAMA Neurol 72:414-22
Cho, Seo-Hyun; Chen, Jason A; Sayed, Faten et al. (2015) SIRT1 deficiency in microglia contributes to cognitive decline in aging and neurodegeneration via epigenetic regulation of IL-1?. J Neurosci 35:807-18
Brambati, Simona Maria; Amici, Serena; Racine, Caroline A et al. (2015) Longitudinal gray matter contraction in three variants of primary progressive aphasia: A tenser-based morphometry study. Neuroimage Clin 8:345-55
Li, Yun; Chen, Jason A; Sears, Renee L et al. (2014) An epigenetic signature in peripheral blood associated with the haplotype on 17q21.31, a risk factor for neurodegenerative tauopathy. PLoS Genet 10:e1004211