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首页> 外文期刊>Fluids and Barriers of the CNS >Circulating tight-junction proteins are potential biomarkers for blood–brain barrier function in a model of neonatal hypoxic/ischemic brain injury
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Circulating tight-junction proteins are potential biomarkers for blood–brain barrier function in a model of neonatal hypoxic/ischemic brain injury

机译:循环紧密结蛋白是新生儿缺氧/缺血性脑损伤模型中血脑屏障功能的潜在生物标志物

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Neonatal encephalopathy often leads to lifelong disabilities with limited treatments currently available. The brain vasculature is an important factor in many neonatal neurological disorders but there is a lack of diagnostic tools to evaluate the brain vascular dysfunction of neonates in the clinical setting. Measurement of blood–brain barrier tight-junction (TJ)?proteins have shown promise as biomarkers for brain injury in the adult. Here we tested the biomarker potential of tight-junctions in the context of neonatal brain injury. The levels of TJ-proteins (occluding, claudin-5, and zonula occludens protein 1) in both blood plasma and cerebrospinal fluid (CSF) as well as blood–brain barrier function via 14C-sucrose (342?Da) and Evans blue extravasation were measured in a hypoxia/ischemia brain-injury model in neonatal rats. Time-dependent changes of occludin and claudin-5 levels could be measured in blood and CSF after hypoxia/ischemia with males generally having higher levels than females. The levels of claudin-5 in CSF correlated with the severity of the brain injury at 24?h post- hypoxia/ischemia. Simultaneously, we detected early increase in blood–brain barrier-permeability at 6 and 24?h after hypoxia/ischemia. Levels of circulating claudin-5 and occludin are increased after hypoxic/ischemic brain injuries and blood–brain barrier-impairment and have promise as early biomarkers for cerebral vascular dysfunction and as a tool for risk assessment of neonatal brain injuries.
机译:新生儿脑病常常导致终身残疾,目前有限的治疗方法。脑血管系统是许多新生儿神经系统疾病的重要因素,但缺乏诊断工具,以评估临床环境中新生儿的脑血管功能障碍。测量血脑屏障紧密交界处(TJ)?蛋白质已经显示为成年人脑损伤的生物标志物。在这里,我们在新生儿脑损伤的背景下测试了紧密连接的生物标志物潜力。通过14C-蔗糖(342〜da)和evans蓝色外渗血浆和脑脊液(CSF)以及血脑屏障功能的TJ-蛋白(CSF)以及血脑屏障功能的水平在新生大鼠的缺氧/缺血脑损伤模型中测量。可以在缺氧/缺血后的血液和CSF中测量occludin和克劳德蛋白-5水平的时间依赖性变化,其缺氧/缺血通常具有比女性更高的含量更高。 CSF中的CLAUDIN-5水平与缺氧/缺血后24μl的脑损伤的严重程度相关。同时,我们在缺氧/缺血后6和24℃下检测到血脑屏障渗透率的早期增加。在缺氧/缺血性脑损伤和血脑障碍损伤后增加循环克劳丁蛋白-5和occludin的水平,并承诺作为脑血管功能障碍的早期生物标志物,并作为新生脑损伤的风险评估的工具。

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