基于 RNA 和单细胞测序数据挖掘鉴定与心肌炎相关的关键 TE

Sixing Chen , Fei Jiang , Jinqiu Wu , Zhi Li , Xiongwei Fan , Xiushan Wu , Yongqing Li , Fang Li , Zhigang Jiang , Yuequn Wang
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摘要

心肌病是一种严重的心脏疾病,其特点是免疫调节机制复杂。虽然免疫基因的作用已得到公认,但它们在心肌病中的具体调控机制还不完全清楚。最近的研究强调了转座元件(TEs)在各种疾病中的重要性,特别是其调节免疫反应的潜力。本文利用可公开获得的数据库来探讨转座元件在心肌炎中的作用:本文分析了 RNA Seq 数据和单细胞测序数据,重点是实验性自身免疫性心肌炎(EAM)小鼠模型。RNA Seq 分析显示,心脏组织中的一系列免疫基因出现了大量上调。利用心脏免疫细胞单细胞测序技术进行的进一步研究发现,某些转座元件(TE)在心脏不同类型的免疫细胞中有特异性表达。此外,ERVB7-1.LTR-MM 转座子在 EAM 模型中各种细胞中的表达量整体增加,表明这种转座子对这种疾病背景下的免疫反应有广泛影响。这项研究的结果突显了心肌病中转座元件与免疫系统之间错综复杂的相互作用,为了解这种疾病的分子机制提供了新的视角。心脏免疫细胞中特异性转座元件表达的发现以及ERVB7-1.LTR-MM 在整个 EAM 模型中表达的增加强调了这些元素在调节免疫反应方面的潜力,有助于我们了解心肌病的发病机制。这些观察结果为进一步研究 TEs 在心脏疾病中的作用开辟了道路,并可能带来新的治疗策略。
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Identification of key TE associated with myocarditis based on RNA and single-cell sequencing data mining

Cardiomyopathy is a severe cardiac condition characterized by complex immune regulatory mechanisms. While the role of immune genes is recognized, the specifics of their regulation in cardiomyopathy are not fully understood. Recent studies highlight the significance of transposable elements (TEs) in various diseases, particularly their potential to modulate immune responses. This paper utilizes publicly available databases to explore the role of TEs in myocarditis: RNA Seq data and single-cell sequencing data were analyzed, with a focus on the mouse model of experimental autoimmune myocarditis (EAM). The RNA-Seq analysis revealed substantial upregulation of a range of immune genes in cardiac tissue. Further investigation using single-cell sequencing of cardiac immune cells identified specific expression of certain transposable elements (TEs) across different types of immune cells in the heart. Additionally, there was an overall increase in the expression of the ERVB7-1. LTR-MM transposon across various cells in the EAM model, suggesting a widespread impact of this transposon on the immune response in this disease context. The findings of this study highlight the intricate interplay between transposable elements and the immune system in cardiomyopathy, providing new insights into the molecular mechanisms underlying this condition. The discovery of specific TEs expression in cardiac immune cells and the overall increase in ERVB7-1. LTR-MM expression across the EAM model underscore the potential of these elements in modulating immune responses and contribute to our understanding of cardiomyopathy's pathogenesis. These observations open avenues for further research into the role of TEs in cardiac disases and may lead to novel therapeutic strategies.

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