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Hydrogen alleviates hyperoxic acute lung injury related endoplasmic reticulum stress in rats through upregulation of SIRT1

机译:氢气减轻了通过SIRT1的上调的大鼠的高氧急性肺损伤相关的内质网胁迫

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摘要

Hyperoxic acute lung injury (HALI) is a major clinical problem for patients undergoing supplemental oxygen therapy. Currently in clinical settings there exist no effective means of prevention or treatment methods. Our previous study found that: hydrogen could reduce HALI, as well as oxidative stress. This research will further explore the mechanism underlying the protective effect of hydrogen on oxygen toxicity. Rats were randomly assigned into three experimental groups and were exposed in a oxygen chamber for 60 continuous hours: 100% balanced air (control); 100% oxygen (HALI); 100% oxygen with hydrogen treatment (HALI+HRS). We examined lung function by wet to dry ratio of lung, lung pleural effusion and cell apoptosis. We also detected endoplasmic reticulum stress (ERS) by examining the expression of CHOP, GRP78 and XBP1. We further investigated the role of Sirtuin 1 (SIRT1) in HALI, which contributes to cellular regulation including ERS, by examining its expression after hydrogen treatment with SIRT1 inhibitor. Hydrogen could significantly reduce HALI by reducing lung edema and apoptosis, inhibiting the elevating of ERS and increased SIRT1 expression. By inhibition of SIRT1 expression, the effect of hydrogen on prevention of HALI is significantly weakened, the inhibition of the ERS was also reversed. Our findings indicate that hydrogen could reduce HALI related ERS and the mechanism of hydrogen may be associated with upregulation of SIRT1, this study reveals the molecular mechanisms underlying the protective effect of hydrogen, which provides a new theoretical basis for clinical application of hydrogen.
机译:高氧急性肺损伤(HALI)是对接受补充氧疗法的患者的主要临床问题。目前在临床环境中,没有有效的预防或治疗方法手段。我们以前的研究发现:氢气可以减少卤素,以及氧化应激。该研究将进一步探讨氢气对氧气毒性保护作用的基础。将大鼠随机分配到三个实验组中,并在氧气室中暴露60个连续时间:100%平衡空气(控制); 100%氧气(卤素); 100%氧气处理(Hali + HRS)。通过湿,肺,肺胸腔积液和细胞凋亡的干比检查肺功能。我们还通过检查CHOP,GRP78和XBP1的表达来检测内质网应激(ERS)。我们进一步研究了SIRTUIN 1(SIRT1)在HALI中的作用,这通过在用SIRT1抑制剂氢处理后检查其表达,这有助于包括ERS的细胞调节。通过减少肺水肿和细胞凋亡,抑制升高的氢气和增加的SIRT1表达,氢气可以显着减少Hali。通过抑制SIRT1表达,氢对预防卤素的效果显着削弱,抑制患者也逆转。我们的研究结果表明,氢气可以减少Hali相关的ERS,并且氢气的机制可能与SIRT1的上调有关,本研究揭示了氢的保护作用的分子机制,为氢气提供了一种新的理论依据。

著录项

  • 来源
    《Free radical research》 |2017年第12期|共11页
  • 作者单位

    PLA Navy Gen Hosp Dept Hyperbar Oxygen 6 Fucheng Rd Beijing 100048 Peoples R China;

    PLA Navy Gen Hosp Dept VIP Respirat Med Beijing Peoples R China;

    PLA Navy Gen Hosp Dept Hyperbar Oxygen 6 Fucheng Rd Beijing 100048 Peoples R China;

    PLA Navy Gen Hosp Dept VIP Respirat Med Beijing Peoples R China;

    PLA Navy Gen Hosp Dept VIP Gen Med Beijing Peoples R China;

    PLA Navy Gen Hosp Dept Hyperbar Oxygen 6 Fucheng Rd Beijing 100048 Peoples R China;

    PLA Navy Gen Hosp Dept Hyperbar Oxygen 6 Fucheng Rd Beijing 100048 Peoples R China;

    PLA Navy Gen Hosp Dept Hyperbar Oxygen 6 Fucheng Rd Beijing 100048 Peoples R China;

    PLA Navy Gen Hosp Dept Hyperbar Oxygen 6 Fucheng Rd Beijing 100048 Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

    Hydrogen; hyperoxic acute lung injury; Sirtuin 1; endoplasmic reticulum stress;

    机译:氢气;高氧急性肺损伤;SIRTUIN 1;内质网胁迫;

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