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Involvement of FOXO Transcription Factors, TRAIL-FasL/Fas, and Sirtuin Proteins Family in Canine Coronavirus Type II-Induced Apoptosis

机译:FOXO转录因子,TRAIL-FasL / Fas和Sirtuin蛋白家族参与犬冠状病毒II型诱导的细胞凋亡。

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摘要

n our previous study, we have shown that canine coronavirus type II (CCoV-II) activates both extrinsic and intrinsic apoptotic pathway in a canine fibrosarcoma cell line (A-72 cells). Herein we investigated the role of Sirtuin and Forkhead box O (FOXO) families in this experimental model using Nortern Blot and Western Blot analysis. Our results demonstrated that mitochondrial SIRT3 and SIRT4 protein expression increased from 12 and 24 h post infection (p.i.) onwards, respectively, whereas the nuclear SIRT1 expression increased during the first 12 h p.i. followed by a decrease after 36 h p.i., reaching the same level of control at 48 h p.i. Sirtuins interact with/and regulate the activity of FOXO family proteins, and we herein observed that FOXO3A and FOXO1 expression increased significantly and stably from 12 h p.i. onwards. In addition, CCoV-II induces a remarkable increase in the expression of TNF-related apoptosis-inducing ligand (TRAIL), while we observed a slight up-regulation of FasL/Fas at 36 p.i. with a decrease of both proteins at the end of infection. Furthermore, we found that virus infection increased both bax translocation into mitochondria and decreased bcl-2 expression in cytosol in a time-dependent manner.
机译:在我们先前的研究中,我们已经显示II型犬冠状病毒(CCoV-II)激活犬纤维肉瘤细胞系(A-72细胞)的外在和内在凋亡途径。本文中,我们使用Nortern Blot和Western Blot分析研究了Sirtuin和Forkhead box O(FOXO)家族在该实验模型中的作用。我们的结果表明,线粒体SIRT3和SIRT4蛋白表达分别从感染后(p.i.)12和24 h开始增加,而核SIRT1表达在p.i的前12 h增加。随后在下午36小时后下降,在下午48小时达到相同的控制水平。 Sirtuins与FOXO家族蛋白相互作用/并调节其活性,我们在本文中观察到FOXO3A和FOXO1的表达自p.i 12小时起显着且稳定地增加。向前。此外,CCoV-II诱导TNF相关凋亡诱导配体(TRAIL)的表达显着增加,而我们在36 p.i观察到FasL / Fas的轻微上调。在感染结束时两种蛋白质均减少。此外,我们发现病毒感染以时间依赖性方式增加了bax易位到线粒体并降低了bcl-2在细胞质中的表达。

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