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首页> 外文期刊>Behavioural Brain Research: An International Journal >The paracrine effect of cobalt chloride on BMSCs during cognitive function rescue in the HIBD rat
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The paracrine effect of cobalt chloride on BMSCs during cognitive function rescue in the HIBD rat

机译:氯化钴对BMSCs在HIBD大鼠中的BMSCs的旁静脉作用

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Hypoxia ischemia (HI)-induced perinatal encephalopathy frequently causes chronic neurological morbidities and acute mortality. Bone mesenchymal stem cell (BMSC) transplantation could potentially promote functional and anatomical recovery of ischemic tissue. In vitro hypoxic preconditioning is an effective strategy to improve the survival of BMSCs in ischemic tissue. In this study, cobalt chloride (CoCl2) preconditioned medium from BMSC cultures was injected into the left lateral ventricle of HI rats using a micro-osmotic pump at a flow rate 1.0 mu l/h for 7 days. The protein levels of HIF-l alpha and its target genes, vascular endothelial growth factor and erythropoietin, markedly increased after CoCl2 preconditioning in BMSCs. In 7-week-old rats that received CoCl2 preconditioned BMSC medium, results of the Morris water maze test indicated ameliorated spatial working memory function following hypoxia-ischemia damage. Neuronal loss, cellular disorganization, and shrinkage in brain tissue were also ameliorated. Extracellular field excitatory postsynaptic potentials (fEPSPs) in the brain slices of 8-week-old rats were recorded; administration of CoCl2 preconditioned BMSC culture medium induced a progressive increment of baseline and amplitude of the fEPSPs. Immunohistochemical quantification showed that GluR2 protein expression increased. In conclusion, CoCl2 activates HIF-la signals in BMSCs. CoCl2 preconditioned BMSC culture medium likely effects neuroprotection by inducing long-term potentiation (LIP), which could be associated with GluR2 expression. The paracrine effects of hypoxia preconditioning on BMSCs could have applications in novel cell-based therapeutic strategies for hypoxic and ischemic brain injury.
机译:缺氧缺血(HI)诱导围产期脑病经常导致慢性神经病症和急性死亡率。骨间充质干细胞(BMSC)移植可能促进缺血组织的功能性和解剖恢复。体外缺氧预处理是改善缺血组织中BMSC的存活的有效策略。在该研究中,使用微渗透泵将来自BMSC培养物的氯化钴(COCl2)预处理培养基使用微渗透泵以1.0μmL/ h以7天的流速注入HI大鼠的左侧肠道。 HIF-Lα及其靶基因,血管内皮生长因子和促红细胞生成素的蛋白质水平明显增加,BMSCs中的COCL2预处理后显着增加。在接受COCl2预处理BMSC培养基的7周龄大鼠中,Morris水迷宫试验的结果表明缺氧缺血损伤后的改善空间工作记忆功能。还改善了神经元损失,细胞紊乱和脑组织的收缩。记录了8周龄大鼠脑切片中的细胞外场兴奋性突触潜力(FEPSP); COCL2预处理BMSC培养基的给药诱导了FEPSPS的基线和幅度的逐渐增加。免疫组织化学定量表明Glur2蛋白表达增加。总之,Cocl2在BMSCs中激活HIF-LA信号。 COCL2预处理BMSC培养基可能通过诱导长期增强(唇)来影响神经保护型,这可能与Glur2表达相关。缺氧对BMSCs的旁慢r次疗效可以具有新的细胞基治疗策略的应用,用于缺氧和缺血性脑损伤。

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