Yu Weihua, Zhang Xiaodi, Liu Jiangzheng, Wang Xin, Li Shuang, Liu Rui, Liao Nai, Zhang Tao, Hai Chunxu
1. Department of Toxicology, the Ministry of Education Key Lab of Hazard Assessment and Control in Special Operational Environment, Shaanxi Provincial Key Lab of Free radical biology and medicine, School of Public Health, The Fourth Military Medical University, Xi'an, 710032, P. R. China.
2. Department of Cardiology, Xijing Hospital, the Fourth Military Medical University, Xi'an, Shaanxi, 710032, China.
Int J Biol Sci. 2016 Jan 1;12(2):198-209. doi: 10.7150/ijbs.13716. eCollection 2016.
P53 is known as a transcription factor to control apoptotic cell death through regulating a series of target genes in nucleus. There is accumulating evidences show that p53 can directly induce cell apoptosis through transcription independent way at mitochondria. However, the mechanism by which p53 translocation into mitochondria in response to oxidative stress remains unclear. Here, glucose oxidase (GOX) was used to induce ROS generation in HepG2 cells and liver tissues of mice. The results showed that p53 was stabilized and translocated to mitochondria in a time and dose dependent manner after GOX exposure. Interestingly, as an inhibitor of mitochondrial permeability transition, cyclosporine A (CsA) was able to effectively reduce GOX mediated mitochondrial p53 distribution without influencing on the expression of p53 target genes including Bcl-2 and Bax. These indicated that CsA could just block p53 entering into mitochondria, but not affect p53-dependent transcription. Meanwhile, CsA failed to inhibit the ROS generation induced by GOX, which indicated that CsA had no antioxidant function. Moreover, GOX induced typical apoptosis characteristics including, mitochondrial dysfunction, accumulation of Bax and release of cytochrome C in mitochondria, accompanied with activation of caspase-9 and caspase-3. These processions were suppressed after pretreatment with CsA and pifithrin-μ (PFT-μ, a specific inhibitor of p53 mitochondrial translocation). In vivo, CsA was able to attenuate p53 mitochondrial distribution and protect mice liver against from GOX mediated apoptotic cell death. Taken together, these suggested that CsA could suppress ROS-mediated p53 mitochondrial distribution and cell apoptosis depended on its inhibition effect to mitochondrial permeability transition. It might be used to rescue the hepatic cell apoptosis in the patients with acute liver injury.
P53作为一种转录因子,通过调控细胞核中的一系列靶基因来控制凋亡性细胞死亡。越来越多的证据表明,p53可通过在线粒体中不依赖转录的方式直接诱导细胞凋亡。然而,p53在氧化应激反应中转位至线粒体的机制仍不清楚。在此,使用葡萄糖氧化酶(GOX)诱导HepG2细胞和小鼠肝脏组织中活性氧(ROS)的产生。结果显示,GOX处理后,p53以时间和剂量依赖性方式被稳定并转位至线粒体。有趣的是,作为线粒体通透性转换的抑制剂,环孢素A(CsA)能够有效减少GOX介导的线粒体p53分布,而不影响包括Bcl-2和Bax在内的p53靶基因的表达。这些结果表明,CsA只能阻止p53进入线粒体,但不影响p53依赖性转录。同时,CsA未能抑制GOX诱导的ROS产生,这表明CsA没有抗氧化功能。此外,GOX诱导了典型的凋亡特征,包括线粒体功能障碍、Bax的积累以及线粒体中细胞色素C的释放,并伴有caspase-9和caspase-3的激活。用CsA和pifithrin-μ(PFT-μ,p53线粒体转位的特异性抑制剂)预处理后,这些过程受到抑制。在体内,CsA能够减弱p53的线粒体分布,并保护小鼠肝脏免受GOX介导的凋亡性细胞死亡。综上所述,这些结果表明CsA可通过其对线粒体通透性转换的抑制作用来抑制ROS介导的p53线粒体分布和细胞凋亡。它可能用于挽救急性肝损伤患者的肝细胞凋亡。
Zotero 插件
