pin1介导的ROS产生参与了n -乙酰- l-半胱氨酸对砷诱导的肝毒性的拮抗作用。

IF 2.2 4区 医学 Q3 TOXICOLOGY
Huijie Zhang, Zhixin He, Ping Deng, Muxue Lu, Chao Zhou, Lingling Yang, Zhengping Yu
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引用次数: 4

摘要

砷是一种广泛存在的环境污染物,对人体多器官具有毒性。暴露于砷会通过过量产生活性氧(ROS)导致肝损伤。PIN1调节ROS水平。n -乙酰- l-半胱氨酸(NAC)是一种保护肝功能的活性氧清除剂。PIN1是否在nac介导的砷肝毒性拮抗中起调节作用仍不清楚。本研究在体外和体内对NAC对砷(NaAsO2)诱导的肝毒性的保护作用进行了评价。砷暴露通过增加细胞内ROS生成、损害线粒体功能和诱导L02肝细胞凋亡诱导细胞毒性。PIN1过表达可显著保护L02细胞免受砷的细胞毒性,降低ROS水平,减轻线粒体功能障碍和凋亡。然而,PIN1的缺失进一步加重了砷诱导的细胞毒性,并消除了NAC在L02细胞中的保护作用。一项体内研究表明,NAC预处理通过恢复肝功能和抑制肝脏氧化应激来挽救砷性肝损伤。转染AAV-Pin1的小鼠过表达PIN1可缓解砷诱导的肝功能障碍和肝脏氧化应激。综上所述,我们的研究确定了PIN1作为拮抗砷诱导肝毒性的新干预靶点,强调了NAC靶向PIN1拮抗砷毒性的新药理学机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

PIN1-mediated ROS production is involved in antagonism of N-acetyl-L-cysteine against arsenic-induced hepatotoxicity.

PIN1-mediated ROS production is involved in antagonism of N-acetyl-L-cysteine against arsenic-induced hepatotoxicity.

Arsenic, a widely existing environmental contaminant, is recognized to be toxic to multiple organs. Exposure to arsenic results in liver damage via excessive production of reactive oxidative species (ROS). PIN1 regulates the levels of ROS. N-acetyl-L-cysteine (NAC) is an ROS scavenger that protects the hepatic functions. Whether PIN1 plays a regulatory role in NAC-mediated antagonism against arsenic hepatotoxicity remains largely unknown. In our study, the protective effects of NAC against arsenic (NaAsO2)-induced hepatotoxicity were evaluated in vitro and in vivo. Arsenic exposure induced cytotoxicity by increasing the intracellular ROS production, impairing mitochondrial function and inducing apoptosis in L02 hepatocytes. Overexpression of PIN1 markedly protected against arsenic cytotoxicity, decreased ROS levels, and mitigated mitochondrial dysfunction and apoptosis in L02 cells. However, loss of PIN1 further aggravated arsenic-induced cytotoxicity and abolished the protective effects of NAC in L02 cells. An in vivo study showed that pretreatment with NAC rescued arsenic-induced liver injury by restoring liver function and suppressing hepatic oxidative stress. Overexpression of PIN1 in mice transfected with AAV-Pin1 relieved arsenic-induced liver dysfunction and hepatic oxidative stress. Taken together, our study identified PIN1 as a novel intervention target for antagonizing arsenic-induced hepatotoxicity, highlighting a new pharmacological mechanism of NAC targeting PIN1 in antagonism against arsenic toxicity.

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来源期刊
Toxicology Research
Toxicology Research TOXICOLOGY-
CiteScore
3.60
自引率
0.00%
发文量
82
期刊介绍: A multi-disciplinary journal covering the best research in both fundamental and applied aspects of toxicology
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