Role of genetic susceptibility variants in predicting clinical course in multiple sclerosis: A cohort study
Version 2 2024-06-03, 18:10Version 2 2024-06-03, 18:10
Version 1 2023-06-19, 05:58Version 1 2023-06-19, 05:58
journal contribution
posted on 2024-06-03, 18:10authored byG 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.