Intermediate CAG Repeat Expansion in the ATXN2 Gene Is a Unique Genetic Risk Factor for ALS−A Systematic Review and Meta-Analysis of Observational Studies

Abstract: Amyotrophic lateral sclerosis (ALS) is a rare degenerative condition of the motor neurons. Over 10% of ALS cases are linked to monogenic mutations, with the remainder thought to be due to other risk factors, including environmental factors, genetic polymorphisms, and possibly gene-environmental interactions. We examined the association between ALS and an intermediate CAG repeat expansion in the ATXN2 gene using a meta-analytic approach. Observational studies were searched with relevant disease and gene terms f… Show more

“…More recently, a large international meta‐analysis of GWAS found 2 loci (at 10q23, SNP rs139550538 and at 1p36, rs2412208) in which the presence of the minor alleles in the homozygous state were significantly associated with a reduction of survival of 7 and 4 months, respectively . Also, the presence of at least 1 minor allele of the rs3011225 SNP located on chromosome 1p34.1 was associated with earlier age of onset in a meta‐analysis of 13 GWAS cohorts . Finally, the presence of an intermediate CAG repeat expansion in the ATXN2 gene not only is a risk factor for ALS but also is associated with a spinal phenotype and reduces survival by 1 year …”

“…28 Also, the presence of at least 1 minor allele of the rs3011225 SNP located on chromosome 1p34.1 was associated with earlier age of onset in a meta-analysis of 13 GWAS cohorts. 29 Finally, the presence of an intermediate CAG repeat expansion in the ATXN2 gene not only is a risk factor for ALS 24 but also is associated with a spinal phenotype and reduces survival by 1 year. 30,31 In summary, we used a large population-based cohort of ALS patients to show that functional variants of the CX3CR1 gene potentially influence ALS survival.…”

Common polymorphisms of chemokine (C‐X3‐C motif) receptor 1 gene modify amyotrophic lateral sclerosis outcome: A population‐based study

“…More recently, a large international meta‐analysis of GWAS found 2 loci (at 10q23, SNP rs139550538 and at 1p36, rs2412208) in which the presence of the minor alleles in the homozygous state were significantly associated with a reduction of survival of 7 and 4 months, respectively . Also, the presence of at least 1 minor allele of the rs3011225 SNP located on chromosome 1p34.1 was associated with earlier age of onset in a meta‐analysis of 13 GWAS cohorts . Finally, the presence of an intermediate CAG repeat expansion in the ATXN2 gene not only is a risk factor for ALS but also is associated with a spinal phenotype and reduces survival by 1 year …”

“…28 Also, the presence of at least 1 minor allele of the rs3011225 SNP located on chromosome 1p34.1 was associated with earlier age of onset in a meta-analysis of 13 GWAS cohorts. 29 Finally, the presence of an intermediate CAG repeat expansion in the ATXN2 gene not only is a risk factor for ALS 24 but also is associated with a spinal phenotype and reduces survival by 1 year. 30,31 In summary, we used a large population-based cohort of ALS patients to show that functional variants of the CX3CR1 gene potentially influence ALS survival.…”

Common polymorphisms of chemokine (C‐X3‐C motif) receptor 1 gene modify amyotrophic lateral sclerosis outcome: A population‐based study

“…The authors went on to describe that the degree of ATXN2 polyglutamine expansion was correlated with the extent of TDP-43 toxicity in both Drosophila and yeast models. Furthermore, ATXN2 intermediate repeat expansion was confirmed as a risk factor in ALS patients [20,106,[144][145][146][147][148][149][150][151][152][153][154][155][156][157][158][159], and more recently as a possible modifier of C9orf72 repeat expansion toxicity in ALS/FTD [107,108].…”

Defining the genetic connection linking amyotrophic lateral sclerosis (ALS) with frontotemporal dementia (FTD)

“…[25] then demonstrated that intermediate (27–33) CAG repeat expansions were present in many ALS patients (henceforth ATXN2 ‐ALS). Two subsequent meta‐analyses of data from a variety of geographical and ethnic backgrounds found increased risk of ALS for CAG repeat lengths of 29–33 [26] and 30–33 [27], respectively.…”

“…Overexpression of TDP-43 is associated with significant cytotoxicity, and thus, levels of this protein are strictly regulated by a number of mechanisms, including an autoregulatory negative feedback loop [24]. On finding that this toxicity was exacerbated by homologues of Ataxin-2 in yeast and flies, Elden et al [25] then demonstrated that intermediate (27)(28)(29)(30)(31)(32)(33) CAG repeat expansions were present in many ALS patients (henceforth ATXN2-ALS). Two subsequent meta-analyses of data from a variety of geographical and ethnic backgrounds found increased risk of ALS for CAG repeat lengths of 29-33 [26] and 30-33 [27], respectively.…”

Motor neurone disease/amyotrophic lateral sclerosis associated with intermediate‐length CAG repeat expansions in Ataxin‐2 does not have 1C2‐positive polyglutamine inclusions