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Valproic Acid Protects Motor Neuron Death by Inhibiting Oxidative Stress and Endoplasmic Reticulum Stress-Mediated Cytochrome C Release after Spinal Cord Injury

机译：丙戊酸通过抑制脊髓损伤后的氧化应激和内质网应激介导的细胞色素C释放来保护运动神经元死亡。

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Both oxidative stress and endoplasmic reticulum (ER) stress are known to contribute to secondary injury, ultimately leading to cell death after spinal cord injury (SCI). Here, we showed that valproic acid (VPA) reduced cell death of motor neurons by inhibiting cytochrome c release mediated by oxidative stress and ER stress after SCI. After SCI, rats were immediately injected with VPA (300 mg/kg) subcutaneously and further injected every 12 h for an indicated time period. Motor neuron cell death at an early time after SCI was significantly attenuated by VPA treatment. Superoxide anion (O2^-) production and inducible NO synthase (iNOS) expression linked to oxidative stress was increased after injury, which was inhibited by VPA. In addition, VPA inhibited c-Jun N-terminal kinase (JNK) activation, which was activated and peaked at an early time after SCI. Furthermore, JNK activation and c-Jun phosphorylation were inhibited by a broad-spectrum reactive oxygen species (ROS) scavenger, Mn (III) tetrakis (4-benzoic acid) porphyrin (MnTBAP), indicating that ROS including O2^- increased after SCI probably contribute to JNK activation. VPA also inhibited cytochrome c release and caspase-9 activation, which was significantly inhibited by SP600125, a JNK inhibitor. The levels of phosphorylated Bim and Mcl-1, which are known as downstream targets of JNK, were significantly reduced by SP600125. On the other hand, VPA treatment inhibited ER stress-induced caspase-12 activation, which is activated in motor neurons after SCI. In addition, VPA increased the Bcl-2/Bax ratio and inhibited CHOP expression. Taken together, our results suggest that cell death of motor neurons after SCI is mediated through oxidative stress and ER stress-mediated cytochrome c release and VPA-inhibited cytochrome c release by attenuating ROS-induced JNK activation followed by Mcl-1 and Bim phosphorylation and ER stress-coupled CHOP expression.

机译：已知氧化应激和内质网应激都可导致继发性损伤，最终导致脊髓损伤（SCI）后细胞死亡。在这里，我们表明丙戊酸（VPA）通过抑制SCI后由氧化应激和ER应激介导的细胞色素C释放来减少运动神经元的细胞死亡。 SCI后，立即给大鼠皮下注射VPA（300μmg/ kg），并在指定的时间间隔内每12h注射一次。 VPA治疗可显着减轻SCI早期的运动神经元细胞死亡。损伤后超氧阴离子（O2 ^{-）的产生和与氧化应激相关的诱导型一氧化氮合酶（iNOS）的表达增加，这被VPA抑制。此外，VPA抑制c-Jun N末端激酶（JNK）活化，该活化在SCI后的早期被激活并达到峰值。此外，JNK活化和c-Jun磷酸化受到广谱活性氧（ROS）清除剂Mn（III）四（4-苯甲酸）卟啉（MnTBAP）的抑制，表明ROS包括O2 ^{-< / sup>在SCI可能有助于JNK激活后增加。 VPA还抑制了细胞色素c的释放和caspase-9的激活，而JNK抑制剂SP600125则明显抑制了该作用。 SP600125显着降低了磷酸化的Bim和Mcl-1的水平，这些水平被称为JNK的下游靶标。另一方面，VPA治疗可抑制ER应力诱导的caspase-12激活，该激活在SCI后在运动神经元中被激活。另外，VPA增加了Bcl-2 / Bax比率并抑制了CHOP表达。两者合计，我们的结果表明，SCI后运动神经元的细胞死亡是通过氧化应激和ER应激介导的细胞色素c释放以及VPA抑制的细胞色素c释放来介导的，其作用是通过减弱ROS诱导的JNK激活，随后Mcl-1和Bim磷酸化以及ER应力耦合的CHOP表达式。}}

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期刊名称 Journal of Neurotrauma
作者
Jee Y. Lee; Sejung Maeng; So R. Kang; Hye Y. Choi; Tae H. Oh; Bong G. Ju; Tae Y. Yune;
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年(卷),期 -1(31),6
年度 -1
页码 582–594
总页数 13
原文格式 PDF
正文语种
中图分类神经科学;神经病学;护理学;
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1. Valproic acid protects motor neuron death by inhibiting oxidative stress and endoplasmic reticulum stress-mediated cytochrome c release after spinal cord injury [J] . LeeJ.Y., MaengS., KangS.R., Journal of neurotrauma . 2014,第6期

机译：丙戊酸通过抑制脊髓损伤后的氧化应激和内质网应激介导的细胞色素C释放来保护运动神经元死亡
2. Panax quinquefolius saponin inhibits endoplasmic reticulum stress-mediated apoptosis and neurite injury and improves functional recovery in a rat spinal cord injury model [J] . Dou Hai-Cheng, Chen Jun-Yu, Ran Tang-Fei, Biomedicine & pharmacotherapy =: Biomedecine & pharmacotherapie . 2018,第期

机译：Panax Quinquefolius Saponin抑制内质网胁迫介导的凋亡和神经突损伤，并提高了大鼠脊髓损伤模型中的功能性恢复
3. Cajaninstilbene acid protects corticosterone-induced injury in PC12 cells by inhibiting oxidative and endoplasmic reticulum stress-mediated apoptosis [J] . Liu Yamin, Shen Shengnan, Li Zongyang, Neurochemistry International: The International Journal for the Rapid Publication of Critical Reviews, Preliminary and Original Research Communications in Neurochemistry . 2014,第Null期

机译：Cajaninstilbene酸通过抑制氧化和内质网应激介导的凋亡来保护皮质酮诱导的PC12细胞损伤
4. GITR-FC Fusion Protein Inhibits GITR Triggering and Protects from the Inflammatory Response Following Spinal Cord Injury [C] . T. Genovese, G. Nocentini, S. Cuzzocrea, Conference on Shock . 2008

机译：GITR-FC融合蛋白抑制GITR触发并保护脊髓损伤后炎症反应免受炎症反应
5. Intermittent hypoxia induces plasticity in spinal synaptic pathways to phrenic motor neurons: A potential therapeutic approach to spinal cord injury? [D] . Lovett-Barr, Mary Rachael. 2008

机译：间歇性缺氧诱导神经运动神经元的脊髓突触途径可塑性：脊髓损伤的潜在治疗方法吗？
6. Nuclear Heme Oxidase-1 Inhibits Endoplasmic Reticulum Stress-Mediated Apoptosis after Spinal Cord Injury [O] . Yunlong Bi, Xi Chen, Yang Cao, 2020

机译：核血红素氧化酶-1抑制脊髓损伤后的内质网胁迫介导的细胞凋亡
7. Increased Expression of a Proline-Rich Akt Substrate (PRAS40) in Human Copper/Zinc-Superoxide Dismutase Transgenic Rats Protects Motor Neurons from Death after Spinal Cord Injury [O] . Fengshan Yu, Purnima Narasimhan, Atsushi Saito, 2007

机译：在人铜/锌 - 超氧化物歧化酶转基因大鼠中增加了富含富含脯氨酸的Akt底物（PRAS40）的表达，保护脊髓损伤后死亡的运动神经元

Valproic Acid Protects Motor Neuron Death by Inhibiting Oxidative Stress and Endoplasmic Reticulum Stress-Mediated Cytochrome C Release after Spinal Cord Injury

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