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首页> 外文期刊>Genes and immunity. >Allelic association of sequence variants in the herpes virus entry mediator-B gene (PVRL2) with the severity of multiple sclerosis.
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Allelic association of sequence variants in the herpes virus entry mediator-B gene (PVRL2) with the severity of multiple sclerosis.

机译:疱疹病毒进入介质-B基因(PVRL2)中序列变体与多发性硬化严重程度的等位关联。

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摘要

Discrepant findings have been reported regarding an association of the apolipoprotein E (APOE) gene with the clinical course of multiple sclerosis (MS). To resolve these discrepancies, we examined common sequence variation in six candidate genes residing in a 380-kb genomic region surrounding and including the APOE locus for an association with MS severity. We genotyped at least three polymorphisms in each of six candidate genes in 1,540 Caucasian MS families (729 single-case and multiple-case families from the United States, 811 single-case families from the UK). By applying the quantitative transmission/disequilibrium test to a recently proposed MS severity score, the only statistically significant (P=0.003) association with MS severity was found for an intronic variant in the Herpes Virus Entry Mediator-B Gene PVRL2. Additional genotyping extended the association to a 16.6 kb block spanning intron 1 to intron 2 of the gene. Sequencing of PVRL2 failed to identify variants with an obvious functional role. In conclusion, the analysis of a very large data set suggests that genetic polymorphisms in PVRL2 may influence MS severity and supports the possibility that viral factors may contribute to the clinical course of MS, consistent with previous reports.
机译:关于载脂蛋白E(APOE)基因与多发性硬化症(MS)临床病程的关联,已报道了不一致的发现。为了解决这些差异,我们检查了居住在380kb基因组区域中的六个候选基因的常见序列变异,这些基因围绕并包括APOE基因座,与MS严重性相关。我们对1,540个白种人MS家族(来自美国的729个单例和多病例家族,来自英国的811个单例家族)的六个候选基因中的至少三个基因型进行了基因分型。通过对最近提出的MS严重度评分应用定量传输/不平衡测试,发现疱疹病毒进入介体B基因PVRL2中内含子变异与MS严重度之间仅有统计学上显着(P = 0.003)的关联。额外的基因分型将关联性扩展到了基因的内含子1至内含子2的16.6 kb区块。 PVRL2的测序未能鉴定出具有明显功能作用的变体。总之,对大量数据的分析表明,PVRL2中的遗传多态性可能影响MS的严重程度,并支持病毒因素可能对MS的临床进程产生影响的可能性,与先前的报道一致。

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