Non-HLA Genes and Multiple Sclerosis

J. Borjac, Alaa Matar, Maxime Merheb, C. Vazhappilly, Rachel Matar
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Abstract

Multiple sclerosis (MS) is an autoimmune demyelinating disease of the central nervous system. Identification of genetic variants that pose risks to MS is of high interest since they contribute largely to disease pathogenesis. A rich body of literature associated these risks with variants of HLA genes located mostly on the short arm of chromosome 6 (6p21). These genetic variations may result in alteration in protein function and are associated, therefore, with disease phenotype and therapy outcome. Although the HLA region has been routinely known to have the strongest correlation with MS, other genes found within and outside HLA locus are considered risk factors for MS. The objective of this review is to shed light on the non-HLA genes implicated with multiple sclerosis. Due to the interplay between the polygenetic and environmental factors, along with their differential contribution and genetic heterogeneity among populations, it is extremely challenging to determine the contribution of the non-HLA genes to the outcome and onset of MS disease. We conclude that a better assemblage of genetic factors involved in MS can have a critical impact on the establishment of a genetic map of MS that allows proper investigation at the expression and functional levels.
非hla基因与多发性硬化症
多发性硬化症(MS)是一种中枢神经系统自身免疫性脱髓鞘疾病。鉴定对多发性硬化症构成风险的遗传变异是高度感兴趣的,因为它们在很大程度上有助于疾病的发病机制。大量文献将这些风险与主要位于6号染色体短臂(6p21)的HLA基因变异联系起来。这些遗传变异可能导致蛋白质功能的改变,因此与疾病表型和治疗结果相关。尽管人们通常认为HLA区域与多发性硬化症的相关性最强,但在HLA位点内外发现的其他基因被认为是多发性硬化症的危险因素。本综述的目的是阐明与多发性硬化症有关的非HLA基因。由于多遗传和环境因素之间的相互作用,以及它们在人群中的差异贡献和遗传异质性,确定非hla基因对MS疾病的结局和发病的贡献是极具挑战性的。我们得出的结论是,更好地组合与多发性硬化症有关的遗传因素可以对建立多发性硬化症的遗传图谱产生关键影响,从而可以在表达和功能水平上进行适当的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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