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儿童皮肌炎的血浆外泌体被人主动脉内皮细胞摄取,并与这些细胞中基因表达的改变有关。

Plasma exosomes from children with juvenile dermatomyositis are taken up by human aortic endothelial cells and are associated with altered gene expression in those cells.

机构信息

Department of Pediatrics, University at Buffalo Jacobs School of Medicine and Biomedical Sciences, Buffalo, NY, USA.

Department of Frontier Medicine, St. Marianna University School of Medicine, Kawasaki, Japan.

出版信息

Pediatr Rheumatol Online J. 2019 Jul 12;17(1):41. doi: 10.1186/s12969-019-0347-0.

Abstract

BACKGROUND

The pathology of juvenile dermatomyositis (JDM) is characterized by prominent vessel wall and perivascular inflammation. This feature of the disease has remained unexplained and under-investigated. We have hypothesized that plasma exosomes, which play an important role in inter-cellular communication, may play a role in the vascular injury associated with JDM.

OBJECTIVE

To characterize the circulating exosomes of children with JDM and determine whether the small RNA cargoes within those exosomes are capable of altering transcriptional programs within endothelial cells.

DESIGN/METHODS: We purified exosomes from plasma samples of children with active, untreated JDM (n = 6) and healthy controls (n = 9). We characterized the small RNA cargoes in JDM and control exosomes by RNA sequencing using the Illumina HiSeq 2500 platform. We then incubated isolated exosomes from healthy controls and children with JDM with cultured human aortic endothelial cells (HAEC) for 24 h. Fluorescence microscopy was used to confirm that both control and JDM exosomes were taken up by HAEC. RNA was then purified from HAEC that had been incubated with either control or JDM exosomes and sequenced on the Illumina platform. Differential expression of mRNAs from HAEC incubated with control or JDM exosomes was ascertained using standard computational methods. Finally, we assessed the degree to which differential gene expression in HAEC could be attributed to the different small RNA cargoes in JDM vs control exosomes using conventional and novel analytic methods.

RESULTS

We identified 10 small RNA molecules that showed differential abundance when we compared JDM and healthy control exosomes. Fluorescence microscopy of labeled exosomes confirmed that both JDM and control exosomes were taken up by HAEC. Differential gene expression analysis revealed 59 genes that showed differential expression between HAEC incubated with JDM exosomes vs HAEC incubated with exosomes from controls. Statistical analysis of gene expression data demonstrated that multiple miRNAs exerted transcriptional control on multiple genes with HAEC.

CONCLUSIONS

Plasma exosomes from children with active, untreated JDM are taken up by HAEC and are associated with alterations in gene expression in those cells. These findings provide new insight into potential mechanisms leading to the targeting of vascular tissue by the immune system in JDM.

摘要

背景

幼年型皮肌炎(JDM)的病理学特征为突出的血管壁和血管周围炎症。该疾病的这一特征尚未得到解释和深入研究。我们假设,在细胞间通讯中发挥重要作用的血浆外泌体可能在与 JDM 相关的血管损伤中发挥作用。

目的

描述 JDM 患儿的循环外泌体,并确定这些外泌体中的小 RNA 货物是否能够改变内皮细胞中的转录程序。

方法/设计:我们从处于活动期、未经治疗的 JDM 患儿(n=6)和健康对照者(n=9)的血浆样本中纯化外泌体。我们使用 Illumina HiSeq 2500 平台通过 RNA 测序来描述 JDM 和对照者外泌体中的小 RNA 货物。然后,我们将来自健康对照者和 JDM 患儿的分离的外泌体与培养的人主动脉内皮细胞(HAEC)共孵育 24 小时。荧光显微镜用于确认 HAEC 摄取了对照者和 JDM 外泌体。然后从与对照者或 JDM 外泌体共孵育的 HAEC 中纯化 RNA,并在 Illumina 平台上进行测序。使用标准计算方法确定与对照者外泌体孵育的 HAEC 中转录物的差异表达。最后,我们使用传统和新型分析方法评估 HAEC 中的差异基因表达在多大程度上归因于 JDM 与对照者外泌体中小 RNA 货物的差异。

结果

我们在比较 JDM 和健康对照者外泌体时发现了 10 种小 RNA 分子的丰度存在差异。标记外泌体的荧光显微镜证实了 JDM 和对照者外泌体均被 HAEC 摄取。差异基因表达分析显示,与 HAEC 与对照者外泌体孵育相比,HAEC 与 JDM 外泌体孵育时有 59 个基因表达差异。基因表达数据的统计分析表明,多个 miRNA 对 HAEC 中的多个基因发挥转录调控作用。

结论

来自处于活动期、未经治疗的 JDM 患儿的血浆外泌体被 HAEC 摄取,并与这些细胞中基因表达的改变相关。这些发现为 JDM 中免疫系统靶向血管组织的潜在机制提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0340/6626431/bd6a0185c6e4/12969_2019_347_Fig1_HTML.jpg

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