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首页> 外文期刊>Brain research bulletin >Corilagin ameliorates sleep deprivation-induced memory impairments by inhibiting NOX2 and activating Nrf2
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Corilagin ameliorates sleep deprivation-induced memory impairments by inhibiting NOX2 and activating Nrf2

机译:Corilagin通过抑制NOx2和激活NRF2来改善睡眠剥夺诱导的记忆障碍

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摘要

Sleep deprivation (SD) can induce cognitive and memory impairments. This impairment is in part due to oxidative stress damage in the hippocampus region of the brain. Corilagin (CL), a polyphenol belonging to the tannin family and extracted from Terminalia chebula and Phyllanthus emblica, shows strong antioxidant and neuroprotective effects. NF-E2-related factor (Nrf2)/heme oxygenase-1 (HO-1) and NADPH oxidase (NOX) are critical targets involved in cellular defense mechanisms against oxidative injury. Thus, we hypothesized that CL could be a preventive treatment for SD-induced memory impairments by inhibiting NOX2 and activating Nrf2. The results from behavioral tests showed that administration of CL resulted in significantly better performance compared to the SD mice. CL significantly normalized the elevated MDA level and the reduced activity of GPx and SOD (P < 0.05, p < 0.01) caused by SD. In hippocampal tissues, CL effectively activated Nrf2/HO-1 signaling and downregulated NOX2 protein expression compared with SD (P < 0.05, P < 0.01). Meanwhile, in vitro findings showed that knockdown of Nrf2 blocked the protective effect of CL versus Glu-induced toxicity, while the effect of CL was enhanced in NOX2 siRNA-transfected neurons. Overall, these findings provided evidence that CL ameliorates SD-induced memory impairments in mice by inhibiting NOX2 and activating Nrf2.
机译:睡眠剥夺(SD)可以诱导认知和记忆障碍。由于大脑的海马区域氧化应激损伤,这种损伤部分是部分原因。属于单宁家族的多酚(CL),从季屈兰氏菌和菲尔氏菌和神经植物源于苯吡喃树脂,显示出强烈的抗氧化剂和神经保护作用。 NF-E2相关系数(NRF2)/血红素氧酶-1(HO-1)和NADPH氧化酶(NOx)是涉及氧化损伤的细胞防御机制的关键目标。因此,我们假设通过抑制NOx2和激活NRF2,CL可以是对SD诱导的记忆损伤的预防性处理。行为试验的结果表明,与SD小鼠相比,Cl的给药导致显着更好的性能。 CL显着归一化MDA水平升高,GPX和SOD的减少活性(P <0.05,P <0.01)引起的SD。在海马组织中,与SD相比,CL有效地活化了NRF2 / HO-1信号和下调的NOX2蛋白表达(P <0.05,P <0.01)。同时,体外发现表明,NRF2的敲低阻断了CL与胶质诱导的毒性的保护作用,而CL的效果在NOx2 siRNA转染的神经元中得到增强。总体而言,这些发现提供了通过抑制NOx2和激活NRF2来改善小鼠中的SD诱导的肠道内存损伤。

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  • 来源
    《Brain research bulletin》 |2020年第1期|共9页
  • 作者单位

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Xian Int Univ Dept Rehabil Med Xian 710077 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

    Fourth Mil Med Univ Xijing Hosp Dept Pharm 127 Changle West St Xian 710032 Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 神经病学与精神病学;
  • 关键词

    Sleep deprivation; Memory impairments; Oxidative stress;

    机译:睡眠剥夺;记忆障碍;氧化应激;

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