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Establishment of an ideal time window model in hypothermic-targeted temperature management after traumatic brain injury in rats

机译:大鼠创伤性脑损伤后低温靶向温度管理理想时间窗模型的建立

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摘要

Although hypothermic-targeted temperature management (HTTM) holds great potential for the treatment of traumatic brain injury (TBI), translation of the efficacy of hypothermia from animal models to TBI patients has no entire consistency. This study aimed to find an ideal time window model in experimental rats which was more in accordance with clinical practice through the delayed HTTM intervention. Sprague-Dawley rats were subjected to unilateral cortical contusion injury and received therapeutic hypothermia at 15 mins, 2 h, 4 h respectively after TBI. The neurological function was evaluated with the modified neurological severity score and Morris water maze test. The brain edema and morphological changes were measured with the water content and H&E staining. Brain sections were immunostained with antibodies against DCX (a neuroblast marker) and GFAP (an astrocyte marker). The apoptosis levels in the ipsilateral hippocampi and cortex were examined with antibodies against the apoptotic proteins Bcl-2, Bax, and cleaved caspase-3 by the immunofluorescence and western blotting. The results indicated that each hypothermia therapy group could improve neurobehavioral and cognitive function, alleviate brain edema and reduce inflammation. Furthermore, we observed that therapeutic hypothermia increased DCX expression, decreased GFAP expression, upregulated Bcl-2 expression and downregulated Bax and cleaved Caspase-3 expression. The above results suggested that HTTM at 2 h or even at 4 h post injury revealed beneficial brain protection similarly, despite the best effect at 15 min post-injury. These findings may provide relatively ideal time window models, further making the following experimental results more credible and persuasive. (C) 2017 Elsevier B.V. All rights reserved.
机译:虽然低温靶向温度管理(HTTM)占治疗创伤性脑损伤(TBI)的潜力巨大,但从动物模型到TBI患者的体温过低的疗效的效果没有整体一致性。本研究旨在在实验大鼠中找到一个理想的时间窗模型,通过延迟HTTM干预,根据临床实践。 Sprague-Dawley大鼠进行单侧皮质挫伤损伤,并在TBI后15分钟,2小时,4小时接受治疗性低温。用改性神经系统严重程度评分和莫里斯水迷宫试验评价神经功能。用含水量和H&E染色测量脑水肿和形态学变化。用针对DCX(神经细胞标记物)和GFAP(星形胶质细胞标记物)的抗体免疫脑切片。通过免疫荧光和蛋白质印迹,用针对凋亡蛋白Bcl-2,Bax和Cleave Caspase-3的抗体检查同侧海马和皮质细胞凋亡水平。结果表明,每个低温治疗组可以改善神经兽医和认知功能,缓解脑水肿并减少炎症。此外,我们观察到治疗性低温增加了DCX表达,降低了GFAP表达,上调的BCL-2表达和下调的BAX并裂解了Caspase-3表达。上述结果表明,HTTM在2小时或甚至在4小时后损伤均显示有益脑保护,尽管损伤后15分钟后效果最佳。这些发现可以提供相对理想的时间窗模型,进一步使以下实验结果更加可信和说服力。 (c)2017 Elsevier B.v.保留所有权利。

著录项

  • 来源
    《Brain research》 |2017年第2017期|共9页
  • 作者单位

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Heart Ctr Tianjin Key Lab Cardiovasc Remodeling &

    Target Or;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Tianjin Univ State Key Lab Precis Measurement Technol &

    Instru Tianjin 300072 Peoples R China;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

    Logist Univ PAPF Pingjin Hosp Tianjin Key Lab Neurotrauma Repair Brain Ctr Tianjin 300162;

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

    Hypothermic-targeted temperature management; Traumatic brain injury; Time window; Effect;

    机译:低温靶向温度管理;创伤性脑损伤;时间窗口;效果;

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