创伤性脑损伤后血脑屏障破坏:创伤后癫痫的可能作用。

Cardiovascular psychiatry and neurology Pub Date : 2011-01-01 Epub Date: 2011-02-22 DOI:10.1155/2011/765923
Oren Tomkins, Akiva Feintuch, Moni Benifla, Avi Cohen, Alon Friedman, Ilan Shelef
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引用次数: 172

摘要

最近的动物实验表明,血脑屏障(BBB)的打开在创伤后癫痫(PTE)的发病机制中起着关键作用。本研究旨在探讨轻度创伤性脑损伤(TBI)后癫痫患者血脑屏障破坏的频率、程度和功能相关性。本研究纳入37例TBI患者,其中19例为PTE,所有患者均行脑电图(EEG)记录和脑磁共振成像(bMRI)检查。脑磁共振成像使用新的定量技术评估血脑屏障破坏。使用标准低分辨率脑电磁断层扫描(sLORETA)定位皮质功能障碍。与对照组相比,TBI患者表现出明显的脑电图减慢,而PTE患者与非癫痫患者之间无显著差异。与25%的非癫痫患者相比,82.4%的PTE患者发现血脑屏障中断(P = 0.001),甚至在创伤后数年也可以观察到。PTE患者伴有血脑屏障破坏的大脑皮质体积明显较大(P = 0.001)。在70%的患者中,慢波脑电图活动定位于血脑屏障破坏的同一区域,并与血脑屏障破坏的皮质体积相关。我们最后提出了一个早期皮层功能障碍和血脑屏障破坏的患者,两种病理逐渐平行解决。我们的研究结果表明,在轻度脑外伤后经常发现血脑屏障病理。在PTE患者中发现持续血脑屏障破裂的频率和程度增加。根据最近的动物研究以及在血脑屏障破坏区域和异常脑电图活动之间发现的共定位,我们认为血管病变在PTE的发病机制中起作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Blood-brain barrier breakdown following traumatic brain injury: a possible role in posttraumatic epilepsy.

Recent animal experiments indicate a critical role for opening of the blood-brain barrier (BBB) in the pathogenesis of post-traumatic epilepsy (PTE). This study aimed to investigate the frequency, extent, and functional correlates of BBB disruption in epileptic patients following mild traumatic brain injury (TBI). Thirty-seven TBI patients were included in this study, 19 of whom suffered from PTE. All underwent electroencephalographic (EEG) recordings and brain magnetic resonance imaging (bMRI). bMRIs were evaluated for BBB disruption using novel quantitative techniques. Cortical dysfunction was localized using standardized low-resolution brain electromagnetic tomography (sLORETA). TBI patients displayed significant EEG slowing compared to controls with no significant differences between PTE and nonepileptic patients. BBB disruption was found in 82.4% of PTE compared to 25% of non-epileptic patients (P = .001) and could be observed even years following the trauma. The volume of cerebral cortex with BBB disruption was significantly larger in PTE patients (P = .001). Slow wave EEG activity was localized to the same region of BBB disruption in 70% of patients and correlated to the volume of BBB disrupted cortex. We finally present a patient suffering from early cortical dysfunction and BBB breakdown with a gradual and parallel resolution of both pathologies. Our findings demonstrate that BBB pathology is frequently found following mild TBI. Lasting BBB breakdown is found with increased frequency and extent in PTE patients. Based on recent animal studies and the colocalization found between the region of disrupted BBB and abnormal EEG activity, we suggest a role for a vascular lesion in the pathogenesis of PTE.

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