14 research outputs found

    Association of Multiple Sclerosis Susceptibility Variants and Early Attack Location in the CNS

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    Objective: The anatomic location of subsequent relapses in early multiple sclerosis (MS) appears to be predicted by the first attack location. We sought to determine if genetic polymorphisms associated with MS susceptibility are associated with attack location. Methods: 17 genome-wide association study-identified MS susceptibility polymorphisms were genotyped in 503 white, non-Hispanic patients seen within a year of MS onset. Their association with the CNS location of the first two MS attacks was assessed in multivariate repeated measures analyses (generalized estimating equations with robust standard errors). Results: The IL12A polymorphism was independently associated with increased odds of attacks involving the spinal cord (OR = 1.52, 95% CI 1.11, 2.07, p = 0.009), as was the IRF8 polymorphism (OR = 2.40, 95% CI [1.04, 5.50], p = 0.040). The IL7R polymorphism was associated with reduced odds of attacks involving the brainstem/cerebellum (OR = 0.46, 95% CI 0.22, 0.97, p = 0.041), as were the TNFRSF1A and IL12A polymorphisms. The CD6 polymorphism conferred reduced odds of optic neuritis as an attack location (OR = 0.69, 95% CI [0.49, 0.97], p = 0.034). Several other genes showed trends for association with attack location. Conclusions: Some of the MS susceptibility genes may be associated with MS attack location. The IL12A polymorphism is of particular interest given that interferon beta therapy appears to influence IL12 levels. These findings may lead to improved understanding of MS pathogenesis and treatment

    Predictors of attack location (multivariate models).

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    <p>Results presented as odds ratios (95% confidence intervals), p values. The analyses take into account first and second attack locations. Of the entire cohort (n = 503), 349 had a second attack. Attack location could not be resolved for 3 initial attacks and 47 second attacks.</p

    Attack severity and recovery.

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    *<p>While 349 in the overall cohort had a second event during follow-up, of those in the CHAMPIONS and ONTT cohorts (total n = 152, 104 (68%) of whom had a second attack), second attack severity was not calculable for ONTT patients and was calculable for 28 (61%) of CHAMPIONS patients who had a second attack. Second attack recovery was calculable for 34 CHAMPIONS patients and no ONTT patient; ** could not be characterized for 2 second events among non-ONTT/non-CHAMPIONS cohorts; *** could not be characterized for 16 first attacks overall or for 11 second events among non-ONTT/non-CHAMPIONS cohorts.</p
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