Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course

BACKGROUND: It remains unclear whether disease course in multiple sclerosis (MS) is influenced by genetic polymorphisms. Here, we aimed to identify genetic variants associated with benign and aggressive disease courses in MS patients. METHODS: MS patients were classified into benign and aggressive p...

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Autores principales: Gil-Varea, Elia, Urcelay, Elena, Vilariño-Güell, Carles, Costa, Carme, Midaglia, Luciana, Matesanz, Fuencisla, Rodríguez-Antigüedad, Alfredo, Oksenberg, Jorge, Espino-Paisan, Laura, Dessa Sadovnick, A., Saiz, Albert, Villar, Luisa M., García-Merino, Juan Antonio, Ramió-Torrentà, Lluís, Triviño, Juan Carlos, Quintana, Ester, Robles, René, Sánchez-López, Antonio, Arroyo, Rafael, Alvarez-Cermeño, Jose C., Vidal-Jordana, Angela, Malhotra, Sunny, Fissolo, Nicolas, Montalban, Xavier, Comabella, Manuel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2018
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6138928/
https://www.ncbi.nlm.nih.gov/pubmed/30217166
http://dx.doi.org/10.1186/s12974-018-1307-1
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author Gil-Varea, Elia
Urcelay, Elena
Vilariño-Güell, Carles
Costa, Carme
Midaglia, Luciana
Matesanz, Fuencisla
Rodríguez-Antigüedad, Alfredo
Oksenberg, Jorge
Espino-Paisan, Laura
Dessa Sadovnick, A.
Saiz, Albert
Villar, Luisa M.
García-Merino, Juan Antonio
Ramió-Torrentà, Lluís
Triviño, Juan Carlos
Quintana, Ester
Robles, René
Sánchez-López, Antonio
Arroyo, Rafael
Alvarez-Cermeño, Jose C.
Vidal-Jordana, Angela
Malhotra, Sunny
Fissolo, Nicolas
Montalban, Xavier
Comabella, Manuel
author_facet Gil-Varea, Elia
Urcelay, Elena
Vilariño-Güell, Carles
Costa, Carme
Midaglia, Luciana
Matesanz, Fuencisla
Rodríguez-Antigüedad, Alfredo
Oksenberg, Jorge
Espino-Paisan, Laura
Dessa Sadovnick, A.
Saiz, Albert
Villar, Luisa M.
García-Merino, Juan Antonio
Ramió-Torrentà, Lluís
Triviño, Juan Carlos
Quintana, Ester
Robles, René
Sánchez-López, Antonio
Arroyo, Rafael
Alvarez-Cermeño, Jose C.
Vidal-Jordana, Angela
Malhotra, Sunny
Fissolo, Nicolas
Montalban, Xavier
Comabella, Manuel
author_sort Gil-Varea, Elia
collection PubMed
description BACKGROUND: It remains unclear whether disease course in multiple sclerosis (MS) is influenced by genetic polymorphisms. Here, we aimed to identify genetic variants associated with benign and aggressive disease courses in MS patients. METHODS: MS patients were classified into benign and aggressive phenotypes according to clinical criteria. We performed exome sequencing in a discovery cohort, which included 20 MS patients, 10 with benign and 10 with aggressive disease course, and genotyping in 2 independent validation cohorts. The first validation cohort encompassed 194 MS patients, 107 with benign and 87 with aggressive phenotypes. The second validation cohort comprised 257 patients, of whom 224 patients had benign phenotypes and 33 aggressive disease courses. Brain immunohistochemistries were performed using disease course associated genes antibodies. RESULTS: By means of single-nucleotide polymorphism (SNP) detection and comparison of allele frequencies between patients with benign and aggressive phenotypes, a total of 16 SNPs were selected for validation from the exome sequencing data in the discovery cohort. Meta-analysis of genotyping results in two validation cohorts revealed two polymorphisms, rs28469012 and rs10894768, significantly associated with disease course. SNP rs28469012 is located in CPXM2 (carboxypeptidase X, M14 family, member 2) and was associated with aggressive disease course (uncorrected p value < 0.05). SNP rs10894768, which is positioned in IGSF9B (immunoglobulin superfamily member 9B) was associated with benign phenotype (uncorrected p value < 0.05). In addition, a trend for association with benign phenotype was observed for a third SNP, rs10423927, in NLRP9 (NLR family pyrin domain containing 9). Brain immunohistochemistries in chronic active lesions from MS patients revealed expression of IGSF9B in astrocytes and macrophages/microglial cells, and expression of CPXM2 and NLRP9 restricted to brain macrophages/microglia. CONCLUSIONS: Genetic variants located in CPXM2, IGSF9B, and NLRP9 have the potential to modulate disease course in MS patients and may be used as disease activity biomarkers to identify patients with divergent disease courses. Altogether, the reported results from this study support the influence of genetic factors in MS disease course and may help to better understand the complex molecular mechanisms underlying disease pathogenesis. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s12974-018-1307-1) contains supplementary material, which is available to authorized users.
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spelling pubmed-61389282018-09-20 Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course Gil-Varea, Elia Urcelay, Elena Vilariño-Güell, Carles Costa, Carme Midaglia, Luciana Matesanz, Fuencisla Rodríguez-Antigüedad, Alfredo Oksenberg, Jorge Espino-Paisan, Laura Dessa Sadovnick, A. Saiz, Albert Villar, Luisa M. García-Merino, Juan Antonio Ramió-Torrentà, Lluís Triviño, Juan Carlos Quintana, Ester Robles, René Sánchez-López, Antonio Arroyo, Rafael Alvarez-Cermeño, Jose C. Vidal-Jordana, Angela Malhotra, Sunny Fissolo, Nicolas Montalban, Xavier Comabella, Manuel J Neuroinflammation Research BACKGROUND: It remains unclear whether disease course in multiple sclerosis (MS) is influenced by genetic polymorphisms. Here, we aimed to identify genetic variants associated with benign and aggressive disease courses in MS patients. METHODS: MS patients were classified into benign and aggressive phenotypes according to clinical criteria. We performed exome sequencing in a discovery cohort, which included 20 MS patients, 10 with benign and 10 with aggressive disease course, and genotyping in 2 independent validation cohorts. The first validation cohort encompassed 194 MS patients, 107 with benign and 87 with aggressive phenotypes. The second validation cohort comprised 257 patients, of whom 224 patients had benign phenotypes and 33 aggressive disease courses. Brain immunohistochemistries were performed using disease course associated genes antibodies. RESULTS: By means of single-nucleotide polymorphism (SNP) detection and comparison of allele frequencies between patients with benign and aggressive phenotypes, a total of 16 SNPs were selected for validation from the exome sequencing data in the discovery cohort. Meta-analysis of genotyping results in two validation cohorts revealed two polymorphisms, rs28469012 and rs10894768, significantly associated with disease course. SNP rs28469012 is located in CPXM2 (carboxypeptidase X, M14 family, member 2) and was associated with aggressive disease course (uncorrected p value < 0.05). SNP rs10894768, which is positioned in IGSF9B (immunoglobulin superfamily member 9B) was associated with benign phenotype (uncorrected p value < 0.05). In addition, a trend for association with benign phenotype was observed for a third SNP, rs10423927, in NLRP9 (NLR family pyrin domain containing 9). Brain immunohistochemistries in chronic active lesions from MS patients revealed expression of IGSF9B in astrocytes and macrophages/microglial cells, and expression of CPXM2 and NLRP9 restricted to brain macrophages/microglia. CONCLUSIONS: Genetic variants located in CPXM2, IGSF9B, and NLRP9 have the potential to modulate disease course in MS patients and may be used as disease activity biomarkers to identify patients with divergent disease courses. Altogether, the reported results from this study support the influence of genetic factors in MS disease course and may help to better understand the complex molecular mechanisms underlying disease pathogenesis. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s12974-018-1307-1) contains supplementary material, which is available to authorized users. BioMed Central 2018-09-14 /pmc/articles/PMC6138928/ /pubmed/30217166 http://dx.doi.org/10.1186/s12974-018-1307-1 Text en © The Author(s). 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Gil-Varea, Elia
Urcelay, Elena
Vilariño-Güell, Carles
Costa, Carme
Midaglia, Luciana
Matesanz, Fuencisla
Rodríguez-Antigüedad, Alfredo
Oksenberg, Jorge
Espino-Paisan, Laura
Dessa Sadovnick, A.
Saiz, Albert
Villar, Luisa M.
García-Merino, Juan Antonio
Ramió-Torrentà, Lluís
Triviño, Juan Carlos
Quintana, Ester
Robles, René
Sánchez-López, Antonio
Arroyo, Rafael
Alvarez-Cermeño, Jose C.
Vidal-Jordana, Angela
Malhotra, Sunny
Fissolo, Nicolas
Montalban, Xavier
Comabella, Manuel
Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
title Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
title_full Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
title_fullStr Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
title_full_unstemmed Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
title_short Exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
title_sort exome sequencing study in patients with multiple sclerosis reveals variants associated with disease course
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6138928/
https://www.ncbi.nlm.nih.gov/pubmed/30217166
http://dx.doi.org/10.1186/s12974-018-1307-1
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