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表观转录组学:HIV 转基因大鼠海马中 N6-甲基腺苷 RNA 甲基化与通路失调的相关性。

Epitranscriptomics: Correlation of N6-methyladenosine RNA methylation and pathway dysregulation in the hippocampus of HIV transgenic rats.

机构信息

Department of Immunology and Microbiology and Department of Neuroscience, The Scripps Research Institute, La Jolla, CA, United States of America.

Department of Pediatrics, Dan L. Duncan Cancer Center, Baylor College of Medicine, Houston, TX, United States of America.

出版信息

PLoS One. 2019 Jan 17;14(1):e0203566. doi: 10.1371/journal.pone.0203566. eCollection 2019.

Abstract

Internal RNA modifications have been known for decades, however their roles in mRNA regulation have only recently started to be elucidated. Here we investigated the most abundant mRNA modification, N6-methyladenosine (m6A) in transcripts from the hippocampus of HIV transgenic (Tg) rats. The distribution of m6A peaks within HIV transcripts in HIV Tg rats largely corresponded to the ones observed for HIV transcripts in cell lines and T cells. Host transcripts were found to be differentially m6A methylated in HIV Tg rats. The functional roles of the differentially m6A methylated pathways in HIV Tg rats is consistent with a key role of RNA methylation in the regulation of the brain transcriptome in chronic HIV disease. In particular, host transcripts show significant differential m6A methylation of genes involved in several pathways related to neural function, suggestive of synaptodendritic injury and neurodegeneration, inflammation and immune response, as well as RNA processing and metabolism, such as splicing. Changes in m6A methylation were usually positively correlated with differential expression, while differential m6A methylation of pathways involved in RNA processing were more likely to be negatively correlated with gene expression changes. Thus, sets of differentially m6A methylated, functionally-related transcripts appear to be involved in coordinated transcriptional responses in the context of chronic HIV. Altogether, our results support that m6A methylation represents an additional layer of regulation of HIV and host gene expression in vivo that contributes significantly to the transcriptional effects of chronic HIV.

摘要

内部 RNA 修饰已经存在了几十年,然而它们在 mRNA 调控中的作用直到最近才开始被阐明。在这里,我们研究了 HIV 转基因(Tg)大鼠海马体中转录本中最丰富的 mRNA 修饰,N6-甲基腺苷(m6A)。HIV Tg 大鼠中转录本中 m6A 峰的分布与在细胞系和 T 细胞中观察到的 HIV 转录本中的分布大致相同。在 HIV Tg 大鼠中,宿主转录本被发现存在差异 m6A 甲基化。HIV Tg 大鼠中差异 m6A 甲基化途径的功能作用与 RNA 甲基化在慢性 HIV 疾病中调节大脑转录组中的关键作用一致。特别是,宿主转录本显示出与几个与神经功能、突触和树突损伤和神经退行性变、炎症和免疫反应以及 RNA 加工和代谢(如剪接)相关的途径相关的基因的显著差异 m6A 甲基化,提示存在突触和树突损伤和神经退行性变、炎症和免疫反应以及 RNA 加工和代谢(如剪接)。m6A 甲基化的变化通常与差异表达呈正相关,而涉及 RNA 加工的途径的差异 m6A 甲基化更可能与基因表达变化呈负相关。因此,在慢性 HIV 情况下,一组差异 m6A 甲基化、功能相关的转录本似乎参与协调转录反应。总之,我们的结果支持 m6A 甲基化代表了 HIV 和宿主基因表达体内调节的另一个层次,它对慢性 HIV 的转录效应有重要贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/69ad/6336335/94e6a2f1773d/pone.0203566.g001.jpg

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