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The neuroprotective effect of picroside II via regulating the expression of myelin basic protein after cerebral ischemia injury in rats

机译:大鼠脑缺血损伤后髓鞘碱性蛋白表达通过调节尿素碱性蛋白表达的神经保护作用

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Background To explore the neuroprotective effect and optimize the therapeutic dose and time window of picroside II by orthogonal test and the expression of myelin basic protein (MBP) in cerebral ischemic injury in rats. Bilateral common carotid artery occlusion (BCCAO) was used to establish forebrain ischemia models. The successful rat models were grouped according to orthogonal experimental design and injected picroside II intraperitoneally at different ischemic time with different doses. Myelin sheath fast green staining(FGS) and transmission electron microscopy (TEM) were used to observe nerve fiber myelin; the expression of MBP was tested qualitatively and quantitatively by immunohistochemical assay (IHC) and Western blot (WB); Reverse transcription polymerase chain reaction (RT-PCR) was used to detect the transcription level of MBP mRNA. Results The protective effect of picroside II was presented by increasing the expression of MBP and decreasing demyelination after cerebral ischemic injury. The best therapeutic time window and dose was (1) ischemia 2.0?h with picroside II 10?mg/kg body weight according to the results of FGS, IHC and WB; (2) ischemia 1.5?h with picroside II 20?mg/kg according to the analysis of RT-PCR. Conclusion Given the principle of the longest time window and the lowest therapeutic dose, the optimized therapeutic dose and time window should be injecting picroside II intraperitoneally with 10-20?mg/kg body weight at ischemia 1.5-2.0?h in cerebral ischemic injury.
机译:背景技术通过正交试验和优化野鸭II的治疗剂量和时间窗和大鼠脑缺血性损伤中髓鞘碱(MBP)的表达和优化醋栗II的治疗剂量和时间窗。双侧常见的颈动脉闭塞(BCOAO)用于建立前脑缺血模型。在不同剂量的不同剂量下,根据正交的实验设计并在不同的缺血时间内腹腔内注射成功的大鼠模型。髓鞘鞘快速绿色染色(FGS)和透射电子显微镜(TEM)用于观察神经纤维髓鞘;通过免疫组织化学测定(IHC)和Western印迹(WB)定性和定量地测试MBP的表达;逆转录聚合酶链反应(RT-PCR)用于检测MBP mRNA的转录水平。结果通过提高MBP的表达和脑缺血性损伤后降低脱髓鞘的表达,提出了野鸭II的保护作用。最佳治疗时间窗和剂量是(1)缺血2.0·H与FGS,IHC和WB的结果的野鸭II 10?Mg / kg体重; (2)根据RT-PCR的分析,尿红素II 20丝葡萄甾醇II 20〜20〜6。结论鉴于最长时间窗口和最低治疗剂量的原理,优化的治疗剂量和时间窗应在脑缺血性损伤中腹腔内用10-20×mg / kg体重注入尿道II。

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