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首页> 外文期刊>Developmental Immunology: Journal of Immunology Research >Unique Gene Expression Patterns in Human T-cell Lines Generated from Multiple Sclerosis Patients by Stimulation with a Synthetic MOG Peptide
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Unique Gene Expression Patterns in Human T-cell Lines Generated from Multiple Sclerosis Patients by Stimulation with a Synthetic MOG Peptide

机译:人工合成MOG肽刺激多发性硬化症患者产生的人类T细胞系中的独特基因表达模式。

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Multiple sclerosis (MS) is an autoimmune disease where T-cells activated against myelin antigens are involved in myelin destruction. Yet, healthy subjects also harbor T-cells responsive to myelin antigens, suggesting that MS patient-derived autoimmune T-cells might bear functional differences from T-cells derived from healthy individuals. We addressed this issue by analyzing gene expression patterns of myelin oligodendrocytic glycoprotein (MOG) responsive T-cell lines generated from MS patients and healthy subjects. We identified 150 transcripts that were differentially expressed between MS patients and healthy controls. The most informative 43 genes exhibited >1.5-fold change in expression level. Eighteen genes were up-regulated including BCL2, lifeguard, IGFBP3 and VEGF. Twenty five genes were down-regulated, including apoptotic activators like TNF and heat shock protein genes. This gene expression pattern was unique to MOG specific T-cell lines and was not expressed in T-cell lines reactive to tetanus toxin (TTX). Our results indicate that activation in MS that promotes T-cell survival and expansion, has its own state and that the unique gene expression pattern that characterize autoreactive T-cells in MS represent a constellation of factors in which the chronicity, timing and accumulation of damage make the difference between health and disease.
机译:多发性硬化症(MS)是一种自身免疫疾病,其中针对髓磷脂抗原激活的T细胞参与了髓磷脂的破坏。然而,健康受试者还带有对髓磷脂抗原有反应的T细胞,这表明MS患者衍生的自身免疫T细胞可能与健康个体的T细胞具有功能差异。我们通过分析由MS患者和健康受试者产生的髓磷脂少突胶质糖蛋白(MOG)反应性T细胞系的基因表达模式来解决此问题。我们鉴定了150个在MS患者和健康对照之间差异表达的转录本。最有用的43个基因在表达水平上表现出> 1.5倍的变化。上调了18个基因,包括BCL2,救生员,IGFBP3和VEGF。下调了25个基因,包括凋亡激活因子(如TNF)和热休克蛋白基因。此基因表达模式是MOG特异性T细胞系所特有的,并且在与破伤风毒素(TTX)具有反应性的T细胞系中未表达。我们的结果表明,MS中的激活可促进T细胞存活和扩增,具有其自身的状态,并且表征MS中自身反应性T细胞的独特基因表达模式代表了一系列因素,其中损伤的长期性,时机和积累使健康与疾病有所不同。

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