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Transcriptomic Profiling of Femoral Veins in Deep Vein Thrombosis in a Porcine Model

机译:猪模型深静脉血栓形成股骨静脉的转录组谱研究

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摘要

Deep vein thrombosis (DVT) is a severe disease affecting the human venous system, accompanied by high morbidity and mortality rates caused by early and late complications. The study aimed at analyzing the changes in the transcriptome of the femoral vein caused by DVT in the porcine model based on the formation of the thrombus in vivo. The study was performed on 11 castrated male pigs: A thrombus was formed in each left femoral vein in six animals; the remaining five served as a control group. Total RNA was isolated from the left femoral veins of the experimental and control animals. High-throughput RNA sequencing was used to analyze the global changes in the transcriptome of veins with induced DVT. Applied multistep bioinformatics revealed 1474 differentially expressed genes (DEGs): 1019 upregulated and 455 downregulated. Functional Gene Ontology annotated 1220 of DEGs into 225 biological processes, 30 molecular functions and 40 cellular components categories. KEGG analysis disclosed TNF, NF-κB and apoptosis pathways’ overexpression in DVT samples. A thorough analysis of the detected DEGs indicated that a dysregulated inflammatory response and disturbed balance between clotting and anti-clotting factors play a crucial role in the process of DVT.
机译:深静脉血栓形成(DVT)是一种严重的疾病,影响人类静脉系统,伴有早期和后期并发症引起的高发病率和死亡率。该研究旨在分析猪模型中DVT引起的股骨静脉转录组的变化,基于体内血栓形成。该研究在11个阉割的雄性猪进行:在六只动物中形成血栓形成血栓;剩下的五个担任对照组。从实验和对照动物的左股骨静脉中分离出总RNA。使用高通量RNA测序分析诱导DVT的静脉转录组的全局变化。施加的MultiStep生物信息学显示1474个差异表达基因(DEGS):1019上调和455下调。功能基因本体在225个生物过程中注释1220,分子功能和40个细胞组分类别。 DVT样品中的TNGG分析公开了TNF,NF-κB和凋亡途径的过度表达。对检测到的DEG的彻底分析表明,凝血和抗凝血因子之间的失调炎症反应和干扰平衡在DVT过程中起重要作用。

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