Linkage, whole genome sequence, and biological data implicate variants in RAB10 in Alzheimer's disease resilience.

Authors

Perry G Ridge
Celeste M Karch
Simon Hsu
Ivan Arano
Craig C Teerlink
Mark T W Ebbert
Josue D Gonzalez Murcia
James M Farnham
Anna R Damato
Mariet Allen
Xue Wang
Oscar Harari
Victoria M Fernandez
Rita Guerreiro
Jose Bras
John Hardy
Ronald Munger
Maria Norton
Celeste Sassi
Andrew Singleton
Steven G Younkin
Dennis W Dickson
Todd E Golde
Nathan D Price, Institute for Systems Biology, 401 Terry Avenue N, Seattle, WAFollow
Nilüfer Ertekin-Taner
Carlos Cruchaga
Alison M Goate
Christopher Corcoran
JoAnn Tschanz
Lisa A Cannon-Albright
John S K Kauwe

Document Type

Article

Publication Date

11-29-2017

Publication Title

Genome Med

Keywords

Aged, 80 and over; Alzheimer Disease; Animals; Brain; Cell Line, Tumor; Female; Gene Expression; Genetic Predisposition to Disease; Humans; Male; Mice; Monomeric GTP-Binding Proteins; Polymorphism, Single Nucleotide; rab GTP-Binding Proteins; Alzheimer’s disease; Linkage analyses; Protective variants; Utah Population Database; Whole genome sequencing

Abstract

BACKGROUND: While age and the APOE ε4 allele are major risk factors for Alzheimer's disease (AD), a small percentage of individuals with these risk factors exhibit AD resilience by living well beyond 75 years of age without any clinical symptoms of cognitive decline.

METHODS: We used over 200 "AD resilient" individuals and an innovative, pedigree-based approach to identify genetic variants that segregate with AD resilience. First, we performed linkage analyses in pedigrees with resilient individuals and a statistical excess of AD deaths. Second, we used whole genome sequences to identify candidate SNPs in significant linkage regions. Third, we replicated SNPs from the linkage peaks that reduced risk for AD in an independent dataset and in a gene-based test. Finally, we experimentally characterized replicated SNPs.

RESULTS: Rs142787485 in RAB10 confers significant protection against AD (p value = 0.0184, odds ratio = 0.5853). Moreover, we replicated this association in an independent series of unrelated individuals (p value = 0.028, odds ratio = 0.69) and used a gene-based test to confirm a role for RAB10 variants in modifying AD risk (p value = 0.002). Experimentally, we demonstrated that knockdown of RAB10 resulted in a significant decrease in Aβ42 (p value = 0.0003) and in the Aβ42/Aβ40 ratio (p value = 0.0001) in neuroblastoma cells. We also found that RAB10 expression is significantly elevated in human AD brains (p value = 0.04).

CONCLUSIONS: Our results suggest that RAB10 could be a promising therapeutic target for AD prevention. In addition, our gene discovery approach can be expanded and adapted to other phenotypes, thus serving as a model for future efforts to identify rare variants for AD and other complex human diseases.

Clinical Institute

Neurosciences (Brain & Spine)

Department

Institute for Systems Biology

Department

Neurosciences

Recommended Citation

Ridge, Perry G; Karch, Celeste M; Hsu, Simon; Arano, Ivan; Teerlink, Craig C; Ebbert, Mark T W; Gonzalez Murcia, Josue D; Farnham, James M; Damato, Anna R; Allen, Mariet; Wang, Xue; Harari, Oscar; Fernandez, Victoria M; Guerreiro, Rita; Bras, Jose; Hardy, John; Munger, Ronald; Norton, Maria; Sassi, Celeste; Singleton, Andrew; Younkin, Steven G; Dickson, Dennis W; Golde, Todd E; Price, Nathan D; Ertekin-Taner, Nilüfer; Cruchaga, Carlos; Goate, Alison M; Corcoran, Christopher; Tschanz, JoAnn; Cannon-Albright, Lisa A; and Kauwe, John S K, "Linkage, whole genome sequence, and biological data implicate variants in RAB10 in Alzheimer's disease resilience." (2017). Articles, Abstracts, and Reports. 552.
https://digitalcommons.providence.org/publications/552