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Role of genetic susceptibility variants in predicting clinical course in multiple sclerosis: A cohort study

Version 2 2024-06-03, 18:10
Version 1 2023-06-19, 05:58
journal contribution
posted on 2024-06-03, 18:10 authored by G Pan, S Simpson, I van der Mei, JC Charlesworth, R Lucas, AL Ponsonby, Y Zhou, F Wu, BV Taylor, K Dear, T Dwyer, L Blizzard, S Broadley, T Kilpatrick, D Williams, J Lechner-Scott, Cameron ShawCameron Shaw, C Chapman, A Coulthard, P Valery
Background The genetic drivers of multiple sclerosis (MS) clinical course are essentially unknown with limited data arising from severity and clinical phenotype analyses in genome-wide association studies. Methods Prospective cohort study of 127 first demyelinating events with genotype data, where 116 MS risk-Associated single nucleotide polymorphisms (SNPs) were assessed as predictors of conversion to MS, relapse and annualised disability progression (Expanded Disability Status Scale, EDSS) up to 5-year review (I "EDSS). Survival analysis was used to test for predictors of MS and relapse, and linear regression for disability progression. The top 7 SNPs predicting MS/relapse and disability progression were evaluated as a cumulative genetic risk score (CGRS). Results We identified 2 non-human leucocyte antigen (HLA; rs12599600 and rs1021156) and 1 HLA (rs9266773) SNP predicting both MS and relapse risk. Additionally, 3 non-HLA SNPs predicted only conversion to MS; 1 HLA and 2 non-HLA SNPs predicted only relapse; and 7 non-HLA SNPs predicted I "EDSS. The CGRS significantly predicted MS and relapse in a significant, dose-dependent manner: Those having ≥5 risk genotypes had a 6-fold greater risk of converting to MS and relapse compared with those with ≤2. The CGRS for I "EDSS was also significant: Those carrying ≥6 risk genotypes progressed at 0.48 EDSS points per year faster compared with those with ≤2, and the CGRS model explained 32% of the variance in disability in this study cohort. Conclusions These data strongly suggest that MS genetic risk variants significantly influence MS clinical course and that this effect is polygenic.

History

Journal

Journal of Neurology, Neurosurgery and Psychiatry

Volume

87

Pagination

1204-1211

Location

London, Eng.

ISSN

0022-3050

eISSN

1468-330X

Language

eng

Publication classification

C1.1 Refereed article in a scholarly journal

Issue

11

Publisher

BMJ Publishing Group

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