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A pilot study of lncRNAs expression profile in serum of progressive multiple sclerosis patients

机译:渐进式多发性硬化症患者血清LNCRNA表达谱的试验研究

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OBJECTIVE: Multiple Sclerosis (MS) is an inflammatory and neurodegenerative disease that affect both white and gray matter. The relapsing and the eventually progressive course of MS is heterogeneous; thus, a confident long-term prediction of individual prognosis is not possible yet. Recent studies have demonstrated the role of long non-coding RNA (lncRNAs) as potential biomarkers that could provide information to predict disease activity and progression. PATIENTS AND METHODS: By qRT-PCR, we analysed the lncRNAs expression in the serum of 16 secondary progressive MS (SP-MS), 12 primary progressive (PP-MS) patients and 8 healthy controls. RESULTS: We found that TUG1 was upregulated in SP-MS, while the comparison of PP-MS vs. controls showed a downregulation of non-protein coding RNA 188 (LRRC75A-AS1) and a significant upregulation of two lncRNAs: long intergenic non-protein coding RNA 293 (LINC00293) and RP11-29G8.3. Moreover, we performed an in-silico analysis using DIANA-LncBase v2 and HMDD v3.0 software, in order to predict the possible interaction of these four lncRNAs with miRNAs. We identified 21 miRNAs prediction targets possibly involved in MS. CONCLUSIONS: Our data indicate a regulatory function of these lncRNAs in autoimmune and inflammatory processes related to MS suggesting their potential role in progressive MS pathogenesis.
机译:目的:多发性硬化症(MS)是一种影响白色和灰质的炎症和神经变性疾病。复发和最终进行MS的渐进过程是异质的;因此,尚未实现对单个预后的自信长期预测。最近的研究表明,长期非编码RNA(LNCRNA)作为潜在生物标志物的作用,可以提供预测疾病活动和进展的信息。患者和方法:通过QRT-PCR,我们分析了16例二次逐步MS(SP-MS),12名初级进展(PP-MS)患者和8例健康对照中的LNCRNA表达。结果:我们发现Tug1在SP-MS中上调,而PP-MS与对照的比较显示非蛋白质编码RNA 188(LRRC75A-AS1)的下调,以及两个LNCRNA的显着上调:长的基础非蛋白质编码RNA 293(LINC00293)和RP11-29G8.3。此外,我们使用Diana-LNCBase V2和HMDD V3.0软件进行了硅基分析,以预测这四种LNCRNA与MIRNA的可能相互作用。我们确定了可能涉及MS的21个miRNA预测目标。结论:我们的数据表明这些LNCRNA在自身免疫和与MS相关的炎症过程中的调节功能,表明其在逐步的MS发病机制中的潜在作用。

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