Genome-Wide Copy Number Variation in Sporadic Amyotrophic Lateral Sclerosis in the Turkish Population: Deletion of EPHA3 Is a Possible Protective Factor

Özgün Uyan,Özgür Ömür,Zeynep Sena Ağım,Filiz Koç,Ersin Tan,Piraye Oflazer,Feza Deymeer,Yeşim Parman,Hong Li,Aslıhan Özoğuz,Hilmi Özçelik,A Nazlı Başak,Mark R Cookson

doi:10.1371/journal.pone.0072381

Abstract

The genome-wide presence of copy number variations (CNVs), which was shown to affect the expression and function of genes, has been recently suggested to confer risk for various human disorders, including Amyotrophic Lateral Sclerosis (ALS). We have performed a genome-wide CNV analysis using PennCNV tool and 733K GWAS data of 117 Turkish ALS patients and 109 matched healthy controls. Case-control association analyses have implicated the presence of both common (>5%) and rare (<5%) CNVs in the Turkish population. In the framework of this study, we identified several common and rare loci that may have an impact on ALS pathogenesis. None of the CNVs associated has been implicated in ALS before, but some have been reported in different types of cancers and autism. The most significant associations were shown for 41 kb and 15 kb intergenic heterozygous deletions (Chr11: 50,545,009–50,586,426 and Chr19: 20,860,930–20,875,787) both contributing to increased risk for ALS. CNVs in coding regions of the MAP4K3, HLA-B, EPHA3 and DPYD genes were detected however, after validation by Log R Ratio (LRR) values and TaqMan CNV genotyping, only EPHA3 deletion remained as a potential protective factor for ALS (p = 0.0065024). Based on the knowledge that EPHA4 has been previously shown to rescue SOD1 transgenic mice from ALS phenotype and prolongs survival, EPHA3 may be a promising candidate for therepuetic interventions.

Highlights

Amyotrophic lateral sclerosis (ALS) is a complex neurodegenerative disorder impacted by genetic and environmental factors
We have investigated for the first time the presence of copy number variations (CNVs) in a Turkish ALS cohort with matched healthy controls; we were able to identify several candidates that may impact the development of ALS in the Turkish population
Values, yielded,25,000 CNV calls with default parameters

Summary

Introduction

Amyotrophic lateral sclerosis (ALS) is a complex neurodegenerative disorder impacted by genetic and environmental factors. To date, using high-density genome-wide single nucleotide polymorphism (SNP) data, four studies restricted to European and US-European ALS populations investigated the presence of CNVs. Cronin et al identified several candidates, including the deletion in C14orf177, and deletion and duplication of the GSDMDC1 and STS genes among 408 Irish and 868 Dutch individuals, respectively [2]. Wain et al analyzed 730 ALS cases and 789 controls to find CNVs associated with ALS They reported several intergenic and gene loci, including two top coding candidates, e.g. duplications of the RDH13 and FBXL2 genes [4]. Blauw et al, conducted a genome-wide screen of 1,875 cases and 8,731 controls (including over 8,000 individuals in replication set), this study revealed deletions and duplications of DPP6 and deletions of NIPA1 loci to be candidates for ALS development [5]

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