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miR-146a 内常见的遗传变异可预测多发性硬化症的发病和复发。

Common genetic variation within miR-146a predicts disease onset and relapse in multiple sclerosis.

机构信息

Menzies Institute for Medical Research, University of Tasmania, 17 Liverpool Street TAS, Hobart, 7000, Australia.

Department of Clinical Laboratory, Xinqiao Hospital, Third Military Medical University, Chongqing, China.

出版信息

Neurol Sci. 2018 Feb;39(2):297-304. doi: 10.1007/s10072-017-3177-1. Epub 2017 Nov 10.

DOI:10.1007/s10072-017-3177-1
PMID:29127522
Abstract

Despite extensive studies focusing on the changes in expression of microRNAs (miRNAs) in multiple sclerosis (MS) compared to healthy controls, few studies have evaluated the association of genetic variants of miRNAs with MS clinical course. We investigated whether a functional polymorphism in the MS associated miR-146a gene predicted clinical course (hazard of conversion to MS and of relapse, and annualized change in disability), using a longitudinal cohort study of persons with a first demyelinating event followed up to their 5-year review. We found the genotype (GC+CC) of rs2910164 predicted relapse compared with the GG genotype (HR=2.09 (95% CI 1.42, 3.06), p=0.0001), as well as a near-significant (p=0.07) association with MS conversion risk. Moreover, we found a significant additive interaction between rs2910164 and baseline anti-EBNA-1 IgG titers predicting risk of conversion to MS (relative excess risk due to interaction [RERI] 2.39, p=0.00002) and of relapse (RERI 1.20, p=0.006). Supporting these results, similar results were seen for the other EBV-correlated variables: anti-EBNA-2 IgG titers and past history of infectious mononucleosis. There was no association of rs2910164 genotype for disability progression. Our findings provide evidence for miR-146a and EBV infection in modulating MS clinical course.

摘要

尽管有大量研究集中在多发性硬化症 (MS) 与健康对照相比,miRNAs (miRNAs) 表达变化,但很少有研究评估 miRNA 遗传变异与 MS 临床病程的相关性。我们通过对首次脱髓鞘事件后随访至 5 年的患者进行纵向队列研究,研究了 MS 相关 miR-146a 基因的功能性多态性是否预测临床病程(转化为 MS 和复发的风险,以及残疾的年变化率)。我们发现 rs2910164 的基因型(GC+CC)与 GG 基因型相比预测复发(HR=2.09(95%CI 1.42, 3.06),p=0.0001),并且与 MS 转化风险有接近显著的关联(p=0.07)。此外,我们发现 rs2910164 与基线抗 EBNA-1 IgG 滴度之间存在显著的相加交互作用,预测转化为 MS 的风险(交互的相对超额风险 [RERI] 2.39,p=0.00002)和复发的风险(RERI 1.20,p=0.006)。支持这些结果,我们还发现其他 EBV 相关变量(抗 EBNA-2 IgG 滴度和既往传染性单核细胞增多症病史)的 EBV 相关变量存在类似的结果。rs2910164 基因型与残疾进展无关。我们的研究结果为 miR-146a 和 EBV 感染在调节 MS 临床病程方面提供了证据。

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