血脑屏障破坏是人类创伤性脑损伤后可能持续多年的早期事件

J. Hay, V. Johnson, A. Young, Douglas H. Smith, W. Stewart
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引用次数: 176

摘要

外伤性脑损伤(TBI)是痴呆的危险因素之一。混合神经退行性病理已被描述为晚期TBI幸存者,但驱动TBI后神经变性的机制仍然难以捉摸。越来越多地,血脑屏障(BBB)的破坏已经在包括痴呆在内的一系列神经系统疾病中被认识到,但对创伤性脑损伤对血脑屏障的影响知之甚少。从格拉斯哥TBI档案(n = 70)中选择单一中度或重度TBI的尸检病例,包括急性(10小时- 13天)到长期(1-47年)生存的范围,以及年龄匹配的未受伤对照(n = 21)。脑外伤后,40%急性期死亡的患者和47%存活一年以上的患者表现出多灶性、异常、血管周围和实质纤维蛋白原和免疫球蛋白G免疫染色,并优先分布于脑回嵴和新皮层深部。相比之下,当存在时,对照组仅显示有限的局部免疫染色。这些初步数据表明,在急性期出现的一部分TBI患者中存在广泛的血脑屏障破坏,有趣的是,在晚期幸存者中持续存在的比例很高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Blood-Brain Barrier Disruption Is an Early Event That May Persist for Many Years After Traumatic Brain Injury in Humans
Abstract Traumatic brain injury (TBI) is a risk factor for dementia. Mixed neurodegenerative pathologies have been described in late survivors of TBI, but the mechanisms driving post-TBI neurodegeneration remain elusive. Increasingly, blood-brain barrier (BBB) disruption has been recognized in a range of neurologic disorders including dementias, but little is known of the consequences of TBI on the BBB. Autopsy cases of single moderate or severe TBI from the Glasgow TBI Archive (n = 70) were selected to include a range from acute (10 hours–13 days) to long-term (1–47 years) survival, together with age-matched uninjured controls (n = 21). Multiple brain regions were examined using immunohistochemistry for the BBB integrity markers fibrinogen and immunoglobulin G. After TBI, 40% of patients dying in the acute phase and 47% of those surviving a year or more from injury showed multifocal, abnormal, perivascular, and parenchymal fibrinogen and immunoglobulin G immunostaining localized to the gray matter, with preferential distribution toward the crests of gyri and deep neocortical layers. In contrast, when present, controls showed only limited localized immunostaining. These preliminary data demonstrate evidence of widespread BBB disruption in a proportion of TBI patients emerging in the acute phase and, intriguingly, persisting in a high proportion of late survivors.
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