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全面分析与动静脉畸形相关的失调外泌体长非编码 RNA 网络。

Comprehensive analysis of dysregulated exosomal long non-coding RNA networks associated with arteriovenous malformations.

机构信息

Department of Interventional Therapy, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, No. 639 Zhi Zao Ju Rd, Shanghai 200011, Shanghai, People's Republic of China.

Department of Department of Oral & Cranio-maxillofacial Surgery, Shanghai Ninth People's Hospital, Shanghai Jiao Tong University School of Medicine, No. 639 Zhi Zao Ju Rd, Shanghai 200011, Shanghai, People's Republic of China.

出版信息

Gene. 2020 May 15;738:144482. doi: 10.1016/j.gene.2020.144482. Epub 2020 Feb 19.

Abstract

Arteriovenous malformations (AVMs) are congenital vascular lesions with a high tendency for aggravation and recurrence after treatment, and their genesis remains enigmatic. In this study, we investigated exosomal long non-coding RNA (lncRNA) and mRNA expression and constructed a competitive endogenous RNA regulatory network in AVMs. Ethics approval was provided, and informed written consent was given prior to the inclusion of all participants. Blood samples were obtained from patients with AVMs and healthy controls at Shanghai Ninth People's Hospital, China, from May to November 2018, and total exosomes were isolated and validated. Differentially expressed exosomal lncRNAs and mRNAs were detected by RNA-seq, analysed by bioinformatic methods and validated by qRT-PCR. A competitive endogenous RNA regulatory network was constructed. The characteristics of the captured extracellular vesicles conformed to the features of exosomes. A total of 117 dysregulated exosomal lncRNAs and 1159 dysregulated exosomal mRNAs were identified in AVMs. qRT-PCR demonstrated that the exosomal lncRNAs MIR4435-1HG, LINC00657, LOC101927854 and SEPT5-GP1BB were upregulated in AVM exosomes. The Gene Ontology (GO) terms haemopoiesis and negative regulation of neuron projection development were significantly enriched in relation to dysregulated exosomal cis lncRNAs. A total of 199 GO terms and 80 Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways were enriched for the dysregulated exosomal mRNAs. In the exosomal lncRNA-miRNA-mRNA-related ceRNA regulatory network, the top 3 significant modules involved 31 dysregulated exosomal lncRNAs and 114 dysregulated exosomal mRNAs, which were enriched in the Rap 1, Ras, MAPK signalling pathways and platelet activation KEGG pathway. This study comprehensively identified dysregulated exosomal lncRNAs and mRNAs in AVMs, demonstrated the involvement of dysregulated lncRNA and mRNA patterns in AVMs and constructed an exosomal competitive endogenous RNA regulatory network.

摘要

动静脉畸形(AVM)是一种先天性血管病变,具有治疗后加重和复发的高倾向,其发生机制仍然神秘。在这项研究中,我们研究了 AVM 中外泌体长链非编码 RNA(lncRNA)和 mRNA 的表达,并构建了 AVM 中的竞争内源性 RNA 调控网络。本研究获得了伦理批准,并在纳入所有参与者之前获得了知情书面同意。2018 年 5 月至 11 月,从中国上海第九人民医院的 AVM 患者和健康对照者中获得血液样本,并分离和验证了总外泌体。通过 RNA-seq 检测差异表达的外泌体 lncRNA 和 mRNA,通过生物信息学方法进行分析,并通过 qRT-PCR 进行验证。构建了竞争内源性 RNA 调控网络。捕获的细胞外囊泡的特征符合外泌体的特征。在 AVM 中发现了 117 个差异表达的外泌体 lncRNA 和 1159 个差异表达的外泌体 mRNA。qRT-PCR 显示,AVM 外泌体中 lncRNA MIR4435-1HG、LINC00657、LOC101927854 和 SEPT5-GP1BB 上调。差异表达的外泌体 cis lncRNA 显著富集了与造血和神经元突起发育负调控相关的基因本体论(GO)术语。差异表达的外泌体 mRNAs 共富集了 199 个 GO 术语和 80 个京都基因与基因组百科全书(KEGG)途径。在外泌体 lncRNA-miRNA-mRNA 相关 ceRNA 调控网络中,前 3 个显著模块涉及 31 个差异表达的外泌体 lncRNA 和 114 个差异表达的外泌体 mRNA,这些模块富集了 Rap1、Ras、MAPK 信号通路和血小板激活 KEGG 通路。本研究全面鉴定了 AVM 中外泌体差异表达的 lncRNA 和 mRNA,证明了失调的 lncRNA 和 mRNA 模式在 AVM 中的参与,并构建了外泌体竞争内源性 RNA 调控网络。

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