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N-n-Butyl Haloperidol Iodide Ameliorates Oxidative Stress in Mitochondria Induced by Hypoxia/Reoxygenation through the Mitochondrial c-Jun N-Terminal Kinase/Sab/Src/Reactive Oxygen Species Pathway in H9c2 Cells

机译：N-正丁基氟哌啶醇碘化物可减轻线粒体c-Jun N末端激酶/ Sab / Src /活性氧物种途径中线粒体c-Jun的缺氧/复氧诱导的线粒体氧化应激

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Both c-Jun N-terminal kinase (JNK) and reactive oxygen species (ROS) play important roles in myocardial ischemia/reperfusion (I/R) injury. Our previous studies suggest that N-n-butyl haloperidol iodide (F2) exerts cardioprotection by reducing ROS production and JNK activation caused by I/R. In this study, we hypothesized that there is a JNK/Sab/Src/ROS pathway in the mitochondria in H9c2 cells following hypoxia/reoxygenation (H/R) that induces oxidative stress in the mitochondria and that F2 exerts mitochondrial protective effects during H/R injury by modulating this pathway. The results showed that H/R induced higher-level ROS in the cytoplasm on the one hand and JNK activation and translocation to the mitochondria by colocalization with Sab on the other. Moreover, H/R resulted in mitochondrial Src dephosphorylation, and subsequently, oxidative stress evidenced by the increase in ROS generation and oxidized cardiolipin in the mitochondrial membranes and by the decrease in mitochondrial superoxide dismutase activity and membrane potential. Furthermore, treatment with a JNK inhibitor or Sab small interfering RNA inhibited the mitochondrial translocation of p-JNK, decreased colocalization of p-JNK and Sab on the mitochondria, and reduced Src dephosphorylation and mitochondrial oxidative stress during H/R. In addition, Src dephosphorylation by inhibitor PP2 increased mitochondrial ROS production. F2, like inhibitors of the JNK/Sab/Src/ROS pathway, downregulated the H/R-induced mitochondrial translocation of p-JNK and the colocalization of p-JNK and Sab on the mitochondria, increased Src phosphorylation, and alleviated the above-mentioned mitochondrial oxidative stress. In conclusion, F2 could ameliorate H/R-associated oxidative stress in mitochondria in H9c2 cells through the mitochondrial JNK/Sab/Src/ROS pathway.

机译：c-Jun N末端激酶（JNK）和活性氧（ROS）都在心肌缺血/再灌注（I / R）损伤中起重要作用。我们以前的研究表明，N-正丁基氟哌啶醇碘化物（F2）通过减少I / R引起的ROS产生和JNK活化来发挥心脏保护作用。在这项研究中，我们假设在缺氧/复氧（H / R）后H9c2细胞的线粒体中存在JNK / Sab / Src / ROS途径，该途径在线粒体中诱导氧化应激，并且F2在H / C期间发挥线粒体保护作用通过调节该途径来R损伤。结果表明，一方面，H / R诱导了细胞质中较高水平的ROS；另一方面，通过与Sab共定位，JNK激活并转移到线粒体。此外，H / R导致线粒体Src脱磷酸化，随后氧化应激由线粒体膜中ROS的产生和氧化型心磷脂的增加以及线粒体超氧化物歧化酶活性和膜电位的降低证明。此外，用JNK抑制剂或Sab小干扰RNA处理可抑制p-JNK的线粒体移位，降低p-JNK和Sab在线粒体上的共定位，并降低H / R期间的Src去磷酸化和线粒体氧化应激。此外，抑制剂PP2的Src脱磷酸作用增加了线粒体ROS的产生。 F2像JNK / Sab / Src / ROS途径的抑制剂一样，下调了H / R诱导的p-JNK的线粒体易位以及p-JNK和Sab在线粒体上的共定位，增加了Src的磷酸化，并减轻了上述影响。提到线粒体的氧化应激。总之，F2可以通过线粒体JNK / Sab / Src / ROS途径减轻H9c2细胞线粒体中与H / R相关的氧化应激。

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期刊名称 Oxidative Medicine and Cellular Longevity
作者
Qianwen Chu; Yanmei Zhang; Shuping Zhong; Fenfei Gao; Yicun Chen; Bin Wang; Zhaojing Zhang; Wenfeng Cai; Weiqiu Li; Fuchun Zheng; Ganggang Shi;
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年(卷),期 2019(2019),-1
年度 2019
页码 7417561
总页数 14
原文格式 PDF
正文语种
中图分类细胞生物学;
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专利

1. N-n-Butyl Haloperidol Iodide Ameliorates Oxidative Stress in Mitochondria Induced by Hypoxia/Reoxygenation through the Mitochondrial c-Jun N-Terminal Kinase/Sab/Src/Reactive Oxygen Species Pathway in H9c2 Cells [J] . Qianwen Chu, Yanmei Zhang, Shuping Zhong, Oxidative Medicine and Cellular Longevity . 2019,第47期

机译：N-正丁基卤代醇碘化物通过线粒体C-JUM N-末端激酶/ SRC /反应性氧气途径在H9C2细胞中通过线粒体C-JUN N-末端激酶/ SAB / SRC /反应性氧气促进氧化胁迫在线粒体中的氧化应激
2. Wenxin Granule Ameliorates Hypoxia/Reoxygenation-Induced Oxidative Stress in Mitochondria via the PKC-δ/NOX2/ROS Pathway in H9c2 Cells [J] . Qihui Jin, Yanhong Jiang, Lizhong Fu, Oxidative Medicine and Cellular Longevity . 2020,第47期

机译：Wenxin颗粒通过H9C2细胞中的PKC-δ/ NOx2 / ROS途径改善了线粒体中的缺氧/释放诱导的氧化胁迫
3. Protoporphyrin IX Induces a Necrotic Cell Death in Human THP-1 Macrophages through Activation of Reactive Oxygen Species/c-Jun N-Terminal Protein Kinase Pathway and Opening of Mitochondrial Permeability Transition Pore [J] . Haobo Xu, Yan Sun, Yun Zhang, Cellular Physiology and Biochemistry . 2014,第6期

机译：原卟啉IX通过活化活性氧/ c-Jun N-末端蛋白激酶途径和线粒体通透性转变孔的开放来诱导人类THP-1巨噬细胞坏死性细胞死亡。
4. Dhhp-6 Protect H9c2 Cardiomyocyte Against Oxidative Injury Induced by Hypoxia/Reoxygenation [C] . Xiaoguang Chen, Lei Huang, Shuwen Guan American Peptide Symposium . 2009

机译：DHHP-6保护H9C2心肌细胞免受缺氧/雷诺诱导的氧化损伤
5. Mitochondrial antioxidants, protection against oxidative stress, and the role of mitochondria in the production of reactive oxygen species. [D] . Rogers, Kara E. 2006

机译：线粒体抗氧化剂，防止氧化应激以及线粒体在产生活性氧方面的作用。
6. Wenxin Granule Ameliorates Hypoxia/Reoxygenation-Induced Oxidative Stress in Mitochondria via the PKC-δ/NOX2/ROS Pathway in H9c2 Cells [O] . Qihui Jin, Yanhong Jiang, Lizhong Fu, 2020

机译：Wenxin颗粒通过H9C2细胞中的PKC-δ/ NOx2 / ROS途径改善了线粒体中的缺氧/释放诱导的氧化胁迫
7. N-n-Butyl Haloperidol Iodide Ameliorates Oxidative Stress in Mitochondria Induced by Hypoxia/Reoxygenation through the Mitochondrial c-Jun N-Terminal Kinase/Sab/Src/Reactive Oxygen Species Pathway in H9c2 Cells [O] . Qianwen Chu, Yanmei Zhang, Shuping Zhong, 2019

机译：N-正丁基卤代醇碘化物通过线粒体C-JUM N-末端激酶/ SRC /反应性氧气途径在H9C2细胞中通过线粒体C-JUN N-末端激酶/ SAB / SRC /反应性氧气促进氧化胁迫在线粒体中的氧化应激

N-n-Butyl Haloperidol Iodide Ameliorates Oxidative Stress in Mitochondria Induced by Hypoxia/Reoxygenation through the Mitochondrial c-Jun N-Terminal Kinase/Sab/Src/Reactive Oxygen Species Pathway in H9c2 Cells

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