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肌萎缩侧索硬化症患者细胞外囊泡和外周血单核细胞的跨组织微小RNA分析

Cross-tissue MiRNA profiling of extracellular vesicles and PBMCs from amyotrophic lateral sclerosis patients.

作者信息

Francesca Dragoni, Rosalinda Di Gerlando, Luca Diamanti, Rizzo Bartolo, Matteo Bordoni, Eveljn Scarian, Viola Camilla, Giovanni Cerchia, Susanna Zucca, Orietta Pansarasa, Stella Gagliardi

机构信息

IRCCS Mondino Foundation, Pavia, Italy.

University of Pavia, Pavia, Italy.

出版信息

Sci Rep. 2025 Apr 29;15(1):14976. doi: 10.1038/s41598-025-99206-2.

Abstract

RNA-mediated toxicity, which can be controlled by alteration of gene expression, is considered a key event in Amyotrophic Lateral Sclerosis (ALS). Transcriptomic deregulation of miRNAs expression can spread via "horizontal" RNA transfer through extracellular vesicles (EVs) to act in conjunction with proteins, leading to changes in mRNA, which can provide early signals to indicate forthcoming neuropathological changes in the brain. The aim of this work is to compare expression profiles (obtained by miRNA-seq) from different tissues to highlight commonly expressed and tissue-specific miRNAs. miRNA species from plasma EVs were correlated with miRNA profiles obtained from peripheral blood mononuclear cells (PBMCs). Each tissue from ALS patients was compared to controls, revealing 159 deregulated (DE) miRNAs in Exosomes (EXOs), 247 DE miRNAs in PBMCs and 162 DE miRNAs in Microvesicles (MVs). Next, data were filtered to include only miRNAs expressed in disease samples (not in healthy subjects), to reduce the number of tissue- and ALS- specific miRNAs (EXO n = 22, MV = 11, PBMCs n = 8). We identified specific miRNAs and pathways related to each tissue. Interestingly, in PBMCs we found mainly neuro-linked pathways, such as neurotransmitters, brain and neuron development, while in EXOs, we found miRNAs implicated in MAPK and ERB signaling. In contrast, the altered pathways in MVs were not specific. This study shows that the composition of small RNA differs significantly between blood cells and its respective EVs fraction. Differentially expressed miRNAs can target definite transcripts in different cellular and molecular fractions. It is evident that, in terms of miRNAs cargo, MVs are not specific to ALS. Therefore, future studies will focus on the interaction between cells and EXOs.

摘要

RNA介导的毒性可通过基因表达的改变来控制,被认为是肌萎缩侧索硬化症(ALS)中的一个关键事件。miRNA表达的转录组失调可通过细胞外囊泡(EVs)进行“水平”RNA转移,并与蛋白质协同作用,导致mRNA发生变化,这可以提供早期信号来指示大脑即将发生的神经病理变化。这项工作的目的是比较不同组织的表达谱(通过miRNA测序获得),以突出共同表达的和组织特异性的miRNA。血浆EVs中的miRNA种类与从外周血单核细胞(PBMCs)获得的miRNA谱相关。将ALS患者的每个组织与对照组进行比较,发现在外泌体(EXOs)中有159个失调(DE)miRNA,在PBMCs中有247个DE miRNA,在微囊泡(MVs)中有162个DE miRNA。接下来,对数据进行筛选,只包括在疾病样本中表达(健康受试者中不表达)的miRNA,以减少组织特异性和ALS特异性miRNA的数量(EXO n = 22,MV = 11,PBMCs n = 8)。我们确定了与每个组织相关的特定miRNA和途径。有趣的是,在PBMCs中,我们主要发现了与神经相关的途径,如神经递质、大脑和神经元发育,而在EXOs中,我们发现了与MAPK和ERB信号传导有关的miRNA。相比之下,MVs中改变的途径并不具有特异性。这项研究表明,血细胞及其各自的EVs部分之间的小RNA组成存在显著差异。差异表达的miRNA可以靶向不同细胞和分子部分中的特定转录本。显然,就miRNA货物而言,MVs对ALS不具有特异性。因此,未来的研究将集中在细胞与EXOs之间的相互作用上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a68d/12041334/fa3c9dd023de/41598_2025_99206_Fig1_HTML.jpg

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