COVID-19 相关急性冠状动脉综合征中的 5-hydroxymethylcytosine 表观遗传标记:中性粒细胞活化和 PDE4D 上调的启示

Zhongheng Li, Maimaitiyasen Duolikun, Hangyu Chen, Lei Zhang, Yishuo Liu, Ruining Li, Dan Li, Long Chen, lijie sun
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摘要

背景:有研究报告称,细胞游离DNA(cfDNA)中的5hmC特征可作为COVID-19发生和发展以及心肌损伤的早期预警生物标志物。然而,其在感染 COVID-19 后急性冠状动脉综合征(ACS)的发生和发展中的作用尚未得到充分研究:首先,我们使用 5hmC-Seal 技术从 24 名 ACS2N 患者(感染 COVID-19 后 2 个月内发病的 ACS 患者)、28 名 ACS2W 患者(感染 COVID-19 后 2 个月后发病的 ACS 患者)和 16 名 ACS 患者(未感染 COVID-19 的 ACS 患者)的血浆 cfDNA 中获得了全基因组 5hmC 图谱。其次,我们对差异表达基因进行了 GO 和 KEGG 分析,发现了一系列与免疫和炎症相关的基因。第三,通过免疫浸润分析研究了不同组别患者免疫细胞的分布情况。最后,我们对这些基因进行了 PPI 网络分析,以确定潜在的关键靶基因:在这项研究中,我们首先发现 ACS2N 患者和 ACS 患者的 5hmC 水平存在显著差异,而 ACS2W 和 ACS 之间的差异并不显著。其次,我们发现 ACS2N 组的中性粒细胞异常活化。最后,通过对差异基因进行 PPI 网络分析,发现 ACS2N 组的靶基因磷酸二酯酶 4D (PDE4D)高表达,并通过外部数据集进行了验证:我们的研究表明,从血浆cfDNA中提取的5hmC标记物可以区分ACS2N和ACS患者。此外,我们还观察到 ACS2N 患者的中性粒细胞表现出异常活化。进一步的分析表明,COVID-19感染可能通过异常上调PDE4D基因的表达而影响ACS的发生和发展。
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5-hydroxymethylcytosine Epigenetic Markers in COVID-19-Associated Acute Coronary Syndrome: Insights into Neutrophil Activation and PDE4D Upregulation
Background: Studies have reported that 5hmC features in cell-free DNA (cfDNA) could serve as early warning biomarkers for the occurrence and progression of COVID-19, as well as myocardial injury. However, its roles in the occurrence and progression of acute coronary syndrome (ACS) following COVID-19 infection has not been fully studied. Methods: Firstly, we used the 5hmC-Seal technique to obtain genome-wide 5hmC profiles from plasma cfDNA of 24 ACS2N patients (individuals experiencing ACS onset within 2 months after COVID-19 infection), 28 ACS2W patients (individuals experiencing ACS onset beyond 2 months after COVID-19 infection), and 16 ACS patients (patients with ACS without COVID-19 infection). Secondly, we performed GO, KEGG analysis on the differentially expressed genes and identified a series of immune and inflammation related genes. Thirdly, the distribution of immune cells in different groups of patients was studied by immune infiltration analysis. Finally, we performed PPI network analysis on these genes to identify potential key target genes. Results: In this study, we firstly found that there was a significant difference in 5hmC levels between ACS2N patients and ACS patients, while the difference between ACS2W and ACS was not significant. Secondly, it was found that neutrophils were abnormally activated in the ACS2N group. Finally, a target gene phosphodiesterase 4D (PDE4D) was found to be highly expressed in the ACS2N group by PPI network analysis of the differential genes and validated with external datasets. Conclusions: Our study suggested that 5hmC markers extracted from plasma cfDNA could differentiate between ACS2N and ACS patients. In addition, we observed that neutrophils exhibited abnormal activation in ACS2N patients. Further analysis showed that COVID-19 infection may affect the occurrence and development of ACS by abnormally up-regulating PDE4D gene expression.
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