Analysis of Neurodegenerative Mendelian Genes in Clinically Diagnosed Alzheimer Disease

Overview

Journal PLoS Genet

Specialty Genetics

Date 2017 Nov 2

PMID 29091718

Citations 22

Authors

Maria Victoria Fernandez

Jong Hun Kim

John P Budde

Kathleen Black

Alexandra Medvedeva

Ben Saef

Yuetiva Deming

Jorge Del-Aguila

Laura Ibanez

Umber Dube

Oscar Harari

Joanne Norton

Rachel Chasse

John C Morris

Alison Goate

Carlos Cruchaga

Affiliations

Soon will be listed here.

Abstract

Alzheimer disease (AD), Frontotemporal lobar degeneration (FTD), Amyotrophic lateral sclerosis (ALS) and Parkinson disease (PD) have a certain degree of clinical, pathological and molecular overlap. Previous studies indicate that causative mutations in AD and FTD/ALS genes can be found in clinical familial AD. We examined the presence of causative and low frequency coding variants in the AD, FTD, ALS and PD Mendelian genes, in over 450 families with clinical history of AD and over 11,710 sporadic cases and cognitive normal participants from North America. Known pathogenic mutations were found in 1.05% of the sporadic cases, in 0.69% of the cognitively normal participants and in 4.22% of the families. A trend towards enrichment, albeit non-significant, was observed for most AD, FTD and PD genes. Only PSEN1 and PINK1 showed consistent association with AD cases when we used ExAC as the control population. These results suggest that current study designs may contain heterogeneity and contamination of the control population, and that current statistical methods for the discovery of novel genes with real pathogenic variants in complex late onset diseases may be inadequate or underpowered to identify genes carrying pathogenic mutations.

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