miR-214/A20表达异常可能在再生障碍性贫血患者的T细胞活化中发挥作用

IF 1.5 Q3 HEMATOLOGY 血液科学(英文) Pub Date : 2020-07-25 eCollection Date: 2020-07-01 DOI:10.1097/BS9.0000000000000053
Zhi Yu, Cunte Chen, Yankai Xiao, Xiaohui Chen, Lixing Guo, Guangxiao Tan, Guixuan Huang, Weifeng Luo, Ming Zhou, Yumiao Li, Chen Lin, Qi Shen, Yuping Zhang, Bo Li
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引用次数: 0

摘要

异常T细胞活化是再生障碍性贫血(AA)发病的主要原因。最近的研究表明,mirna调节T细胞活化并参与AA。先前的一项研究发现,miR-214通过靶向PTEN以cd28依赖的方式在T细胞活化时显著上调。然而,miR-214及其靶基因在AA中的表达特征尚未明确。在本研究中,miR-214的靶基因通过生物信息学和荧光素酶报告基因检测预测和确认。采用实时定量逆转录聚合酶链反应检测36例健康人及35例AA患者外周血单个核细胞中miR-214及靶基因的表达水平。生物信息学和荧光素酶报告基因检测发现,miR-214可以结合到a203 '非翻译区。与健康组相比,AA患者miR-214显著升高,A20表达水平显著降低。此外,与严重再生障碍性贫血患者相比,非重度再生障碍性贫血患者miR-214明显升高。这些结果表明,A20基因是miR-214的潜在靶标,miR-214的升高可能至少在一定程度上通过调节A20在AA中的表达来激活T细胞。我们首先证实了miR-214调控A20的表达,miR-214/A20的异常表达可能与AA的免疫病理有关。miR-214的表达可能作为一种潜在的生物标志物,有助于诊断AA的严重程度。
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Abnormal miR-214/A20 expression might play a role in T cell activation in patients with aplastic anemia.

Aberrant T cell activation is a major cause of aplastic anemia (AA) pathogenesis. Recent studies have shown that miRNAs regulate T cell activation and are involved in AA. A previous study found that miR-214 was significantly up-regulated upon T cell activation in a CD28-dependent fashion by targeting PTEN. However, the expression characteristics of miR-214 and its target genes in AA have not been defined. In this study, target genes for miR-214 were predicted and confirmed by bioinformatics and luciferase reporter assays. The expression levels of miR-214 and target genes were detected in 36 healthy individuals and 35 patients with AA in peripheral blood mononuclear cells by real-time quantitative reverse transcriptase-polymerase chain reaction. Bioinformatics and luciferase reporter assays identified that miR-214 could bind to the A20 3' untranslated regions. Significantly increased miR-214 and the decreased A20 expression level were detected in the AA patients compared with the healthy group. In addition, significantly increased miR-214 was found in non-severe aplastic anemia compared with severe aplastic anemia patients. These results suggested that the A20 gene was a potential target of miR-214, and elevated miR-214 might medicate T cell activation at least in part by regulating A20 expression in AA. We firstly confirmed that miR-214 regulated A20 expression, and aberrant miR-214/A20 expression might contribute to immunopathology in AA. The miR-214 expression might be used as a potential biomarker that assisted in diagnosing AA severity.

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