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The whole transcriptome and proteome changes in the early stage of myocardial infarction

机译:心肌梗死早期整个转录组和蛋白质组的变化

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摘要

As the most severe manifestation of coronary artery disease, myocardial infarction (MI) is a complex and multifactorial pathophysiologic process. However, the pathogenesis that underlies MI remains unclear. Here, we generated a MI mouse model by ligation of the proximal left anterior descending coronary artery. The transcriptome and proteome, at different time points after MI, were detected and analysed. Immune-related pathways, cell cycle-related pathways, and extracellular matrix remodelling-related pathways were significantly increased after MI. Not only innate immune cells but also adaptive immune cells participated in the early stage of MI. Proteins that functioned in blood agglutination, fibrinolysis, secretion, and immunity were significantly changed after MI. Nppa, Serpina3n, and Anxa1, three secreted proteins that can easily be detected in blood, were significantly changed after MI. Our discoveries not only reveal the molecular and cellular changes in MI but also identify potential candidate biomarkers of MI for clinical diagnosis or treatment.
机译:心肌梗死(MI)是冠状动脉疾病最严重的表现,是一个复杂而多因素的病理生理过程。但是,尚不清楚MI的发病机理。在这里,我们通过结扎左前降支冠状动脉近端产生了MI小鼠模型。检测并分析心肌梗死后不同时间点的转录组和蛋白质组。 MI后免疫相关途径,细胞周期相关途径和细胞外基质重塑相关途径明显增加。不仅先天免疫细胞而且适应性免疫细胞也参与了MI的早期阶段。 MI后,在血液凝集,纤维蛋白溶解,分泌和免疫中起作用的蛋白质发生了显着变化。 MI后,Nppa,Serpina3n和Anxa1这三种在血液中容易检测到的分泌蛋白发生了显着变化。我们的发现不仅揭示了MI的分子和细胞变化,而且还鉴定了MI的潜在候选生物标志物,用于临床诊断或治疗。

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