Centro de Biología Molecular "Severo Ochoa", CSIC-UAM, Univ, Autónoma de Madrid, Madrid, Spain.
J Neuroinflammation. 2012 Jul 2;9:157. doi: 10.1186/1742-2094-9-157.
Estradiol has been shown to exert neuroprotective effects in several neurodegenerative conditions, including cerebral ischemia. The presence of this hormone prior to ischemia attenuates the damage associated with such events in a rodent model (middle cerebral artery occlusion (MCAO)), although its therapeutic value when administered post-ischemia has not been assessed. Hence, we evaluated the effects of estradiol treatment after permanent MCAO (pMCAO) was induced in rats, studying the PI3K/AKT/GSK3/β-catenin survival pathway and the activation of SAPK-JNK in two brain areas differently affected by pMCAO: the cortex and hippocampus. In addition, we analyzed the effect of estradiol on the glial response to injury.
Male rats were subjected to pMCAO and estradiol (0.04 mg/kg) was administered 6, 24, and 48 h after surgery. The animals were sacrificed 6 h after the last treatment, and brain damage was evaluated by immunohistochemical quantification of 'reactive gliosis' using antibodies against GFAP and Iba1. In addition, Akt, phospho-Akt(Ser473), phospho-Akt(Thr308), GSK3, phospho-GSK3(Ser21/9), β-catenin, SAPK-JNK, and pSAPK-JNK(Thr183/Tyr185) levels were determined in western blots of the ipsilateral cerebral cortex and hippocampus, and regional differences in neuronal phospho-Akt expression were determined by immunohistochemistry.
The increases in the percentage of GFAP- (5.25-fold) and Iba1- (1.8-fold) labeled cells in the cortex and hippocampus indicate that pMCAO induced 'reactive gliosis'. This effect was prevented by post-ischemic estradiol treatment; diminished the number of these cells to those comparable with control animals. pMCAO down-regulated the PI3K/AkT/GSK3/β-catenin survival pathway to different extents in the cortex and hippocampus, the activity of which was restored by estradiol treatment more efficiently in the cerebral cortex (the most affected region) than in the hippocampus. No changes in the phosphorylation of SAPK-JNK were observed 54 h after inducing pMCAO, whereas pMCAO did significantly decrease the phospho-Akt(Ser473) in neurons, an effect that was reversed by estradiol.
The present study demonstrates that post-pMCAO estradiol treatment attenuates ischemic injury in both neurons and glia, events in which the PI3K/AKT/GSK3/β-catenin pathway is at least partly involved. These findings indicate that estradiol is a potentially useful treatment to enhance recovery after human ischemic stroke.
雌二醇已被证明在几种神经退行性疾病中具有神经保护作用,包括脑缺血。在啮齿动物模型(大脑中动脉闭塞(MCAO))中,这种激素在缺血前存在可减轻与此类事件相关的损伤,尽管其在缺血后给药的治疗价值尚未评估。因此,我们评估了在大鼠中诱导永久性 MCAO(pMCAO)后,雌二醇治疗的效果,研究了 PI3K/AKT/GSK3/β-连环蛋白存活途径以及 SAPK-JNK 在两个受 pMCAO 影响不同的脑区中的激活:皮质和海马。此外,我们分析了雌二醇对神经胶质细胞对损伤反应的影响。
雄性大鼠接受 pMCAO,术后 6、24 和 48 小时给予雌二醇(0.04mg/kg)。最后一次治疗后 6 小时处死动物,通过针对 GFAP 和 Iba1 的免疫组织化学定量来评估“反应性神经胶质增生”来评估脑损伤。此外,通过 Western blot 测定同侧大脑皮质和海马中的 Akt、磷酸化 Akt(Ser473)、磷酸化 Akt(Thr308)、GSK3、磷酸化 GSK3(Ser21/9)、β-连环蛋白、SAPK-JNK 和 pSAPK-JNK(Thr183/Tyr185)水平,并通过免疫组织化学测定神经元磷酸化 Akt 的区域差异。
皮质和海马中 GFAP(5.25 倍)和 Iba1(1.8 倍)标记细胞的百分比增加表明 pMCAO 诱导了“反应性神经胶质增生”。这种作用被缺血后雌二醇治疗所预防;将这些细胞的数量减少到与对照动物相当的水平。pMCAO 在皮质和海马中不同程度地下调了 PI3K/Akt/GSK3/β-连环蛋白存活途径,而雌二醇处理在大脑皮质(受影响最严重的区域)中更有效地恢复了该途径的活性,而在海马中则不然。在诱导 pMCAO 后 54 小时未观察到 SAPK-JNK 磷酸化的变化,而 pMCAO 显著降低了神经元中的磷酸化 Akt(Ser473),这一作用被雌二醇逆转。
本研究表明,pMCAO 后给予雌二醇可减轻神经元和神经胶质细胞的缺血性损伤,其中 PI3K/AKT/GSK3/β-连环蛋白途径至少部分参与其中。这些发现表明,雌二醇是增强人类缺血性中风后恢复的一种潜在有用的治疗方法。
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