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早期骨髓单核细胞移植通过旁分泌机制促进癫痫持续状态后小鼠的神经保护和炎症调节。

Early transplantation of bone marrow mononuclear cells promotes neuroprotection and modulation of inflammation after status epilepticus in mice by paracrine mechanisms.

机构信息

Hospital São Rafael, Av. São Rafael, 2152. São Marcos, Salvador, BA, 41253-190, Brazil.

出版信息

Neurochem Res. 2014 Feb;39(2):259-68. doi: 10.1007/s11064-013-1217-7. Epub 2013 Dec 17.

DOI:10.1007/s11064-013-1217-7
PMID:24343530
Abstract

Status epilepticus (SE) is a severe clinical manifestation of epilepsy associated with intense neuronal loss and inflammation, two key factors involved in the pathophysiology of temporal lobe epilepsy. Bone marrow mononuclear cells (BMMC) attenuated the consequences of pilocarpine-induced SE, including neuronal loss, in addition to frequency and duration of seizures. Here we investigated the effects of BMMC transplanted early after the onset of SE in mice, as well as the involvement of soluble factors produced by BMMC in the effects of the cell therapy. Mice were injected with pilocarpine for SE induction and randomized into three groups: transplanted intravenously with 1 × 10(7) BMMC isolated from GFP transgenic mice, injected with BMMC lysate, and saline-treated controls. Cell tracking, neuronal counting in hippocampal subfields and cytokine analysis in the serum and brain were performed. BMMC were found in the brain 4 h following transplantation and their numbers progressively decreased until 24 h following transplantation. A reduction in hippocampal neuronal loss after SE was found in mice treated with live BMMC and BMMC lysate when compared to saline-treated, SE-induced mice. Moreover, the expression of inflammatory cytokines IL-1β, TNF-α, IL-6 was decreased after injection of live BMMC and to a lesser extent, of BMMC lysate, when compared to SE-induced controls. In contrast, IL-10 expression was increased. Analysis of markers for microglia activation demonstrated a reduction of the expression of genes related to type 1-activation. BMMC transplantation promotes neuroprotection and mediates anti-inflammatory effects following SE in mice, possibly through the secretion of soluble factors.

摘要

癫痫持续状态(SE)是癫痫的一种严重临床表现,与强烈的神经元丧失和炎症有关,这两个因素是颞叶癫痫发病机制中的关键因素。骨髓单核细胞(BMMC)减轻了匹鲁卡品诱导的 SE 的后果,包括神经元丧失,以及癫痫发作的频率和持续时间。在这里,我们研究了 SE 发作后早期移植 BMMC 对小鼠的影响,以及 BMMC 产生的可溶性因子在细胞治疗中的作用。将小鼠用匹鲁卡品注射以诱导 SE,并随机分为三组:静脉注射来自 GFP 转基因小鼠的 1×10(7) BMMC、注射 BMMC 裂解物和生理盐水处理的对照组。进行细胞追踪、海马亚区神经元计数和血清及脑组织细胞因子分析。移植后 4 小时在脑中发现 BMMC,其数量逐渐减少,直到移植后 24 小时。与生理盐水处理、SE 诱导的小鼠相比,用活 BMMC 和 BMMC 裂解物处理的 SE 后,海马神经元丧失减少。此外,与 SE 诱导的对照组相比,注射活 BMMC 和 BMMC 裂解物后,促炎细胞因子 IL-1β、TNF-α、IL-6 的表达减少,而 IL-10 的表达增加。对小胶质细胞激活标志物的分析表明,与 1 型激活相关的基因的表达减少。BMMC 移植可促进 SE 后小鼠的神经保护和介导抗炎作用,可能通过分泌可溶性因子。

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