Epilepsy Research Laboratory, A.I. Virtanen Institute for Molecular Sciences, University of Kuopio, PO Box 1627, FIN-70211 Kuopio, Finland.
Neuroscience. 2010 Mar 10;166(1):312-32. doi: 10.1016/j.neuroscience.2009.12.002. Epub 2009 Dec 23.
Angiogenesis and blood-brain-barrier (BBB) damage have been proposed to contribute to epileptogenesis and/or ictogenesis in experimental and human epilepsy. We tested a hypothesis that after brain injury angiogenesis occurs in the most damaged hippocampal areas with the highest need of tissue repair, and associates with formation of epileptogenic neuronal networks. We induced status epilepticus (SE) with pilocarpine in adult rats, and investigated endothelial cell proliferation (BrdU and rat endothelial cell antigen-1 (RECA-1) double-labeling), vessel length (unbiased stereology), thrombocyte aggregation (thrombocyte immunostaining), neurodegeneration (Nissl staining), neurogenesis (doublecortin (DCX) immunohistochemistry), and mossy fiber sprouting (Timm staining) in the hippocampus at different time points post-SE. As functional measures we determined BBB leakage (quantified immunoglobulin G (IgG) immunostaining), and hippocampal blood volume (CBV) and flow (CBF) in vivo (magnetic resonance imaging, MRI). The total length of hippocampal blood vessels was decreased by 17% at 2 d after status epilepticus (SE) induced by pilocarpine in adult rats (P<0.05 as compared to controls) which was not accompanied by alterations in hippocampal blood volume (BV) and flow (BF). Number of proliferating endothelial cells peaked at 4 d post-SE and correlated with an increase in vessel length (r=0.900, P<0.05). Vessels length had recovered to control level or even higher at 2 wk post-SE, angiogenesis being most prominent in the CA3 (128% as compared to that in controls, P<0.05), and was associated with increased BV (178% as compared to that in controls, P<0.05). Enlargement of vessel diameter in the hippocampal fissure was associated with thrombocyte aggregation in distal capillaries. BBB was most leaky during the first 4 d post-SE and increased IgG extravasation was observed for 60 d. Our data show that magnitude of endothelial cell proliferation is not associated with severity of acute post-SE neurodegeneration or formation of abnormal neuronal network. This encourages identification of molecular targets that initiate and maintain specific aspects of tissue reorganization, including preservation and proliferation of endothelial cells to reduce the risk of epileptogenesis and enhance recovery after brain injury.
血管生成和血脑屏障 (BBB) 损伤被认为有助于实验性和人类癫痫中的癫痫发生和/或发作形成。我们检验了一个假设,即在脑损伤后,血管生成发生在最受损的海马区域,这些区域最需要组织修复,并与致痫性神经网络的形成相关。我们用匹罗卡品诱导成年大鼠癫痫持续状态 (SE),并在 SE 后不同时间点检测海马内皮细胞增殖 (BrdU 和大鼠内皮细胞抗原-1 (RECA-1) 双重标记)、血管长度 (无偏立体学)、血小板聚集 (血小板免疫染色)、神经退行性变 (尼氏染色)、神经发生 (双皮质素 (DCX) 免疫组织化学) 和苔藓纤维发芽 (Timm 染色)。作为功能测量,我们在体内 (磁共振成像,MRI) 测定了 BBB 渗漏 (定量 IgG 免疫染色)和海马血容量 (CBV) 和血流 (CBF)。用匹罗卡品诱导成年大鼠 SE 后 2 天,海马血管总长度减少 17% (与对照组相比,P<0.05),但海马血容量 (BV) 和血流 (BF) 没有改变。增殖内皮细胞数量在 SE 后 4 天达到峰值,并与血管长度的增加相关 (r=0.900,P<0.05)。SE 后 2 周,血管长度已恢复至对照水平甚至更高,血管生成在 CA3 最为明显 (与对照组相比,增加 128%,P<0.05),并与 BV 增加相关 (与对照组相比,增加 178%,P<0.05)。海马裂血管直径增大与远端毛细血管血小板聚集有关。SE 后第 1 至 4 天 BBB 渗漏最严重,60 天观察到 IgG 外渗。我们的数据表明,内皮细胞增殖的程度与 SE 后急性期神经退行性变的严重程度或异常神经网络的形成无关。这鼓励确定启动和维持组织重构特定方面的分子靶点,包括保留和增殖内皮细胞,以降低癫痫发生的风险并增强脑损伤后的恢复。
