Quantitative proteomic analysis reveals regulatory networks of extracellular matrix receptor interaction pathways in endothelial cells after myocardial infarction

Xuan Wu, Jiageng Cai, Peng Wang, Lingyun Zu
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Abstract

Cardiac fibrosis, a significant pathological alteration following myocardial infarction (MI), remains enigmatic with respect to the role of cardiac endothelial cells (ECs). To elucidate the proteomic shifts in cardiac ECs accompanying MI-induced cardiac fibrosis, a standard MI mice model was established through ligation of the left anterior descending branch. Following 14 days of effective modeling, we isolated primary ECs from the hearts of both sham and MI models utilizing the CD31 microbeads sorting technique. Quantitative proteomics and bioinformatics methodologies, including tandem mass spectrometry, were employed to discern proteomic alterations in the primary endothelial cells of the experimental groups. Comprehensive analyses, including Gene Ontology analysis, Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis, functional enrichment analysis, and functional enrichment cluster analysis, revealed an up-regulation of proteins associated with extracellular matrix-receptor interaction pathway in cardiac fibrosis post-MI. Subsequent Western blot analysis confirmed the up-regulation of specific proteins involved in this pathway, namely collagen type VI alpha 2 (Col6α2), vitronectin (Vtn), and integrin beta (Itgβ). We conclude that the expression levels of Col6α2, Vtn, and Itgβ in primary ECs during the early stage of cardiac fibrosis, 14 days post-MI, were significantly elevated compared to the sham group (P < 0.05). This observation suggests that ECM-receptor interaction could potentially influence the progression of cardiac fibrosis following MI.
定量蛋白质组分析揭示心肌梗死后血管内皮细胞细胞外基质受体相互作用通路的调控网络
心脏纤维化是心肌梗死(MI)后的一种重要病理改变,但心脏内皮细胞(ECs)的作用仍是一个谜。为了阐明心肌梗死诱发心脏纤维化后心脏内皮细胞蛋白质组的变化,我们通过结扎左前降支建立了标准的心肌梗死小鼠模型。经过 14 天的有效建模后,我们利用 CD31 微珠分选技术从假性和 MI 模型的心脏中分离出了原发性心 ECs。我们采用定量蛋白质组学和生物信息学方法(包括串联质谱法)来鉴别实验组原代内皮细胞的蛋白质组学变化。基因本体分析、京都基因和基因组百科全书(KEGG)分析、功能富集分析和功能富集聚类分析等综合分析表明,在心肌梗死后的心脏纤维化中,与细胞外基质-受体相互作用通路相关的蛋白质上调。随后的 Western 印迹分析证实了参与该通路的特定蛋白的上调,即Ⅵ型胶原α2(Col6α2)、玻璃连蛋白(Vtn)和整合素β(Itgβ)。我们得出结论:与假组相比,在心肌梗死后 14 天的心脏纤维化早期,原发性心肌中 Col6α2、Vtn 和 Itgβ 的表达水平显著升高(P < 0.05)。这一观察结果表明,ECM 与受体的相互作用可能会影响心肌梗死后心脏纤维化的进展。
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