TY - JOUR
T1 - Contribution of Rare and Low-Frequency Variants to Multiple Sclerosis Susceptibility in the Italian Continental Population
AU - PROGEMUS
AU - PROGRESSO
AU - Clarelli, Ferdinando
AU - Barizzone, Nadia
AU - Mangano, Eleonora
AU - Zuccalà, Miriam
AU - Basagni, Chiara
AU - Anand, Santosh
AU - Sorosina, Melissa
AU - Mascia, Elisabetta
AU - Santoro, Silvia
AU - Guerini, Franca Rosa
AU - Virgilio, Eleonora
AU - Gallo, Antonio
AU - Pizzino, Alessandro
AU - Comi, Cristoforo
AU - Martinelli, Vittorio
AU - Comi, Giancarlo
AU - De Bellis, Gianluca
AU - Leone, Maurizio
AU - Filippi, Massimo
AU - Esposito, Federica
AU - Bordoni, Roberta
AU - Martinelli Boneschi, Filippo
AU - D'Alfonso, Sandra
N1 - Publisher Copyright:
Copyright © 2022 Clarelli, Barizzone, Mangano, Zuccalà, Basagni, Anand, Sorosina, Mascia, Santoro, Guerini, Virgilio, Gallo, Pizzino, Comi, Martinelli, Comi, De Bellis, Leone, Filippi, Esposito, Bordoni, Martinelli Boneschi and D'Alfonso.
PY - 2022/1/3
Y1 - 2022/1/3
N2 - Genome-wide association studies identified over 200 risk loci for multiple sclerosis (MS) focusing on common variants, which account for about 50% of disease heritability. The goal of this study was to investigate whether low-frequency and rare functional variants, located in MS-established associated loci, may contribute to disease risk in a relatively homogeneous population, testing their cumulative effect (burden) with gene-wise tests. We sequenced 98 genes in 588 Italian patients with MS and 408 matched healthy controls (HCs). Variants were selected using different filtering criteria based on allelic frequency and in silico functional impacts. Genes showing a significant burden (n = 17) were sequenced in an independent cohort of 504 MS and 504 HC. The highest signal in both cohorts was observed for the disruptive variants (stop-gain, stop-loss, or splicing variants) located in EFCAB13, a gene coding for a protein of an unknown function (p < 10–4). Among these variants, the minor allele of a stop-gain variant showed a significantly higher frequency in MS versus HC in both sequenced cohorts (p = 0.0093 and p = 0.025), confirmed by a meta-analysis on a third independent cohort of 1298 MS and 1430 HC (p = 0.001) assayed with an SNP array. Real-time PCR on 14 heterozygous individuals for this variant did not evidence the presence of the stop-gain allele, suggesting a transcript degradation by non-sense mediated decay, supported by the evidence that the carriers of the stop-gain variant had a lower expression of this gene (p = 0.0184). In conclusion, we identified a novel low-frequency functional variant associated with MS susceptibility, suggesting the possible role of rare/low-frequency variants in MS as reported for other complex diseases.
AB - Genome-wide association studies identified over 200 risk loci for multiple sclerosis (MS) focusing on common variants, which account for about 50% of disease heritability. The goal of this study was to investigate whether low-frequency and rare functional variants, located in MS-established associated loci, may contribute to disease risk in a relatively homogeneous population, testing their cumulative effect (burden) with gene-wise tests. We sequenced 98 genes in 588 Italian patients with MS and 408 matched healthy controls (HCs). Variants were selected using different filtering criteria based on allelic frequency and in silico functional impacts. Genes showing a significant burden (n = 17) were sequenced in an independent cohort of 504 MS and 504 HC. The highest signal in both cohorts was observed for the disruptive variants (stop-gain, stop-loss, or splicing variants) located in EFCAB13, a gene coding for a protein of an unknown function (p < 10–4). Among these variants, the minor allele of a stop-gain variant showed a significantly higher frequency in MS versus HC in both sequenced cohorts (p = 0.0093 and p = 0.025), confirmed by a meta-analysis on a third independent cohort of 1298 MS and 1430 HC (p = 0.001) assayed with an SNP array. Real-time PCR on 14 heterozygous individuals for this variant did not evidence the presence of the stop-gain allele, suggesting a transcript degradation by non-sense mediated decay, supported by the evidence that the carriers of the stop-gain variant had a lower expression of this gene (p = 0.0184). In conclusion, we identified a novel low-frequency functional variant associated with MS susceptibility, suggesting the possible role of rare/low-frequency variants in MS as reported for other complex diseases.
KW - EFCAB13
KW - burden test
KW - multiple sclerosis
KW - pool sequencing
KW - rare variants
UR - http://www.scopus.com/inward/record.url?scp=85123090989&partnerID=8YFLogxK
U2 - 10.3389/fgene.2021.800262
DO - 10.3389/fgene.2021.800262
M3 - Article
SN - 1664-8021
VL - 12
JO - Frontiers in Genetics
JF - Frontiers in Genetics
M1 - 800262
ER -