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系统性红斑狼疮患者B细胞亚群的MicroRNA分析揭示了有前景的新型生物标志物。

MicroRNA Profiling of B Cell Subsets from Systemic Lupus Erythematosus Patients Reveals Promising Novel Biomarkers.

作者信息

Duroux-Richard Isabelle, Cuenca Jimena, Ponsolles Clara, Piñeiro Alejandro Badilla, Gonzalez Fernando, Roubert Christine, Areny Roser, Chea Rosa, Pefaur Jacqueline, Pers Yves-Marie, Figueroa Fernando E, Jorgensen Christian, Khoury Maroun, Apparailly Florence

机构信息

INSERM, U1183, Institute of Regenerative Medicine and Biotherapy, University Hospital Saint Eloi, Montpellier 34295, France.

University of Montpellier, Montpellier 34090, France.

出版信息

Int J Mol Sci. 2015 Jul 27;16(8):16953-65. doi: 10.3390/ijms160816953.

Abstract

MicroRNAs control the differentiation and function of B cells, which are considered key elements in the pathogenesis of systemic lupus erythematosus (SLE). However, a common micro(mi)RNA signature has not emerged since published data includes patients of variable ethnic background, type of disease, and organ involvement, as well as heterogeneous cell populations. Here, we aimed at identifying a miRNA signature of purified B cells from renal and non-renal severe SLE patients of Latin American background, a population known to express severe disease. Genome-wide miRNA expression analyses were performed on naive and memory B cells and revealed two categories of miRNA signatures. The first signature represents B cell subset-specific miRNAs deregulated in SLE: 11 and six miRNAs discriminating naive and memory B cells of SLE patients from healthy controls (HC), respectively. Whether the miRNA was up or down-regulated in memory B cells as compared with naive B cells in HC, this difference was abolished in SLE patients, and vice versa. The second signature identifies six miRNAs associated with specific pathologic features affecting renal outcome, providing a further understanding for SLE pathogenesis. Overall, the present work provided promising biomarkers in molecular diagnostics for disease severity as well as potential new targets for therapeutic intervention in SLE.

摘要

微小RNA控制B细胞的分化和功能,而B细胞被认为是系统性红斑狼疮(SLE)发病机制中的关键因素。然而,由于已发表的数据涵盖了不同种族背景、疾病类型和器官受累情况的患者,以及异质性细胞群体,因此尚未出现常见的微小(mi)RNA特征。在此,我们旨在鉴定来自拉丁美洲背景的肾脏和非肾脏重症SLE患者纯化B细胞的miRNA特征,该群体以表达严重疾病而闻名。对初始B细胞和记忆B细胞进行了全基因组miRNA表达分析,揭示了两类miRNA特征。第一个特征代表SLE中失调的B细胞亚群特异性miRNA:分别有11个和6个miRNA可区分SLE患者与健康对照(HC)的初始B细胞和记忆B细胞。与HC中记忆B细胞相比,初始B细胞中miRNA是上调还是下调,在SLE患者中这种差异消失了,反之亦然。第二个特征鉴定出与影响肾脏结局的特定病理特征相关的6个miRNA,为SLE发病机制提供了进一步的理解。总体而言,本研究为疾病严重程度的分子诊断提供了有前景的生物标志物,以及SLE治疗干预的潜在新靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/801a/4581178/11390abff151/ijms-16-16953-g001.jpg

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