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Transcriptome analysis of common and diverged circulating miRNAs between arterial and venous during aging

机译:老化期间动脉和静脉常见循环miRNA的转录组分析

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摘要

Circulating miRNAs have received extensive attention as non-invasive biomarkers for prediction and diagnosis of disease. However, most samples have been obtained from peripheral venous blood. To evaluate whether peripheral venous miRNAs represent circulating miRNAs from all blood vessels under a given condition, such as aging, we compared the miRNA profiles of venous and arterial plasma between young and aged rats by Illumina next-generation sequencing. The DEseq2 tool was used to obtain differentially-expressed miRNAs. We observed 105 aging-related deregulated miRNAs in vein and 62 in artery, which were highly associated with cell survival and inflammation, respectively. On the other hand, the young and aged groups exhibited a unique arterial-venous bias. There were 54 differentially-expressed miRNAs in the young group and 42 in the aged group; only 8 miRNAs were shared. Further transcriptional factors enrichment analysis found that the shared miRNAs could be partially upregulated by NF-κB and SIRT1. These transcriptional factors could be organ-specific and/or regulated in physiological and aging states as possible causal factors. This study suggested the potential application of circulating miRNAs, which reflect the systematic response to certain conditions, such as aging, and the importance of origin selection for candidate circulating miRNAs.
机译:循环miRNA作为非侵入性生物标志物的广泛关注,用于预测和诊断疾病。然而,大多数样品已经从外周静脉血液中获得。为了评估外周静脉MIRNA是否代表来自给定条件的所有血管的循环miRNA,例如老化,通过Illumina下一代测序比较了年轻和老年大鼠之间的静脉和动脉血浆的miRNA谱。 DESEQ2工具用于获得差异表达的miRNA。我们观察到静脉中的105例与静脉62中的衰老病毒的MiRNA分别与细胞存活和炎症高度相关。另一方面,年轻和老年的团体表现出独特的动脉静脉偏见。年轻组中有54名差异表达的miRNA,42岁左右;仅共享8名miRNA。进一步的转录因子富集分析发现,共享miRNA可以通过NF-κB和SIRT1部分上调。这些转录因子可能是在生理和老化状态下的器官特异性和/或受管制的因因素。该研究表明循环miRNA的潜在应用,这反映了对某些条件的系统反应,例如老化,以及原产地选择候选循环miRNA的原点选择的重要性。

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