miR-138作为系统性硬化症新诊断生物标志物的异常表达

IF 3.4 Q2 MEDICINE, RESEARCH & EXPERIMENTAL Biomarker Insights Pub Date : 2022-01-01 DOI:10.1177/11772719221135442
Paria Bayati, Hadi Poormoghim, Nazanin Mojtabavi
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引用次数: 4

摘要

背景:MicroRNAs是一种短核苷酸序列,有助于调节各种生物功能,因此它们在许多病理条件下的作用已被研究,如癌症和纤维化中的上皮细胞向间质细胞转化;其中,miR-138在癌症生物学领域的研究最多,因其对癌症进展的抑制作用而闻名。miR-138能够抑制参与EMT的主要途径,也可能是纤维化反应研究的一个很好的候选者。基于我们之前的研究,以及miR-138靶向和调节EMT通路的几个组分的能力;我们假设miR-138在系统性硬化症中的作用。因此,评估miR-138的基因表达,以发现SSc患者全血中的任何改变。方法:采集70例系统性硬化症患者的血液(分为局限性组和弥漫性组)和30例健康人作为对照。立即从新鲜全血中分离RNA;然后将得到的RNA逆转录成cDNA,通过qPCR、特异性TaqMan引物和探针比较患者与对照组miR-138的相对表达量。结果:与对照组相比,系统性硬化症患者miR-138的相对表达明显降低。局限性组和弥漫性组之间无显著差异。ROC曲线分析显示miR-138在有效区分SSc患者与健康对照中具有适当的诊断价值。结论:miR-138可能参与了SSc的发病机制,经过进一步的评估,miR-138可能被用作SSc的诊断生物标志物。此外,在未来的研究中靶向miR-138可能有望为SSc患者找到一种新的治疗选择。
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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Aberrant expression of miR-138 as a novel diagnostic biomarker in systemic sclerosis.

Background: MicroRNAs are short nucleotide sequences that contribute to the regulation of various biological functions and therefore their roles have been investigated in many pathologic conditions such as epithelial to mesenchymal transition in cancer and fibrosis; among them, miR-138 has been mostly studied in cancer biology and is well-known for its suppressing effect on cancer progression. Being able to suppress major pathways involved in EMT, miR-138 could be a good candidate to be investigated in fibrotic responses too. Based on our previous studies, and the capability of miR-138 to target and regulate several components of the EMT pathway; we hypothesized a role for miR-138 in systemic sclerosis. Accordingly, the gene expression of miR-138 was assessed to find any alterations in the whole blood of the SSc patients.

Methods: Blood was collected from 70 patients with systemic sclerosis (equally divided between 2 groups of limited and diffuse categories) and 30 healthy individuals as controls. RNA was immediately isolated from the fresh whole blood; afterward, the resulting RNA was reverse transcribed into cDNA and then the relative expression of miR-138 was compared between the patients and the controls by the means of qPCR, and specific TaqMan primer and probes.

Results: The relative expression of miR-138 was significantly lower in patients with systemic sclerosis compared to the controls. No significant difference was observed between the limited and diffuse patient groups. ROC curve analysis showed an appropriate diagnostic value of miR-138 in effectively differentiating SSc patients from the healthy controls.

Conclusion: miR-138 is likely involved in the pathogenesis of SSc and with further evaluations may be utilized as a diagnostic biomarker in SSc. Also, targeting miR-138 in future studies could be promising for finding a novel treatment option for patients with SSc.

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来源期刊
Biomarker Insights
Biomarker Insights MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
6.00
自引率
0.00%
发文量
26
审稿时长
8 weeks
期刊介绍: An open access, peer reviewed electronic journal that covers all aspects of biomarker research and clinical applications.
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