No rare deleterious variants from STK32B, PPARGC1A, and CTNNA3 are associated with essential tremor

Author:

Houle Gabrielle,Ambalavanan Amirthagowri,Schmouth Jean-François,Leblond Claire S.,Spiegelman Dan,Laurent Sandra B.,Bourassa Cynthia V.,Grayson Celene,Panisset Michel,Chouinard Sylvain,Dupré Nicolas,Vilariño-Güell Carles,Rajput Alex,Girard Simon L.,Dion Patrick A.,Rouleau Guy A.

Abstract

Objective:To assess the contribution of variants in STK32B, PPARGC1A, and CTNNA3 as essential tremor (ET) predisposing factors following their association in a 2-stage genome-wide association study (GWAS).Methods:The coding regions of these genes was examined for the presence of rare variants using two approaches: (1) Looking at whole-exome and whole-genome sequencing data of 14 autosomal dominant multiplex ET families. (2) Conducting a targeted massive parallel sequencing to examine the three genes in cohorts of 269 ET cases and 287 control individuals. The cumulative impact of rare variants was assessed using SKAT-O analyses using (1) all variants, (2) only rare variants, and (3) only the rare variants altering the mRNA.Results:Thirty-four variants were identified. No difference emerged regarding the distributions of individual variants (or gene) between cases and controls.Conclusion:No rare exonic variants further validated one of these genes as a risk factor for ET. The recent GWAS offers promising avenues, but the genetic heterogeneity of ET is nonetheless challenging for the validation of risk factors, and ultimately larger cohorts of cases should help to overcome this task.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Genetics (clinical),Neurology (clinical)

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