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首页> 外文期刊>Journal of neuroinflammation >Immunomodulatory effect of Hawthorn extract in an experimental stroke model
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Immunomodulatory effect of Hawthorn extract in an experimental stroke model

机译:山楂提取物在实验性中风模型中的免疫调节作用

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Background Recently, we reported a neuroprotective effect for Hawthorn (Crataegus oxyacantha) ethanolic extract in middle cerebral artery occlusion-(MCAO) induced stroke in rats. The present study sheds more light on the extract's mechanism of neuroprotection, especially its immunomodulatory effect. Methods After 15 days of treatment with Hawthorn extract [100 mg/kg, pretreatment (oral)], male Sprague Dawley rats underwent transient MCAO for 75 mins followed by reperfusion (either 3 or 24 hrs). We measured pro-inflammatory cytokines (IL-1β, TNF-α, IL-6), ICAM-1, IL-10 and pSTAT-3 expression in the brain by appropriate methods. We also looked at the cytotoxic T cell sub-population among leukocytes (FACS) and inflammatory cell activation and recruitment in brain (using a myeloperoxidase activity assay) after ischemia and reperfusion (I/R). Apoptosis (TUNEL), and Bcl-xL- and Foxp3- (Treg marker) positive cells in the ipsilateral hemisphere of the brain were analyzed separately using immunofluorescence. Results Our results indicate that occlusion followed by 3 hrs of reperfusion increased pro-inflammatory cytokine and ICAM-1 gene expressions in the ipsilateral hemisphere, and that Hawthorn pre-treatment significantly (p ≤ 0.01) lowered these levels. Furthermore, such pre-treatment was able to increase IL-10 levels and Foxp3-positive cells in brain after 24 hrs of reperfusion. The increase in cytotoxic T cell population in vehicle rats after 24 hrs of reperfusion was decreased by at least 40% with Hawthorn pretreatment. In addition, there was a decrease in inflammatory cell activation and infiltration in pretreated brain. Hawthorn pretreatment elevated pSTAT-3 levels in brain after I/R. We also observed an increase in Bcl-xL-positive cells, which in turn may have influenced the reduction in TUNEL-positive cells compared to vehicle-treated brain. Conclusions In summary, Hawthorn extract helped alleviate pro-inflammatory immune responses associated with I/R-induced injury, boosted IL-10 levels, and increased Foxp3-positive Tregs in the brain, which may have aided in suppression of activated inflammatory cells. Such treatment also minimizes apoptotic cell death by influencing STAT-3 phosphorylation and Bcl-xL expression in the brain. Taken together, the immunomodulatory effect of Hawthorn extract may play a critical role in the neuroprotection observed in this MCAO-induced stroke model.
机译:背景技术最近,我们报道了山楂(Crataegus oxyacantha)乙醇提取物对大鼠大脑中动脉阻塞(MCAO)所致中风的神经保护作用。本研究为提取物的神经保护机制,特别是其免疫调节作用提供了更多的启示。方法用山楂提取物[100 mg / kg,预处理(口服)]治疗15天后,对雄性Sprague Dawley大鼠进行短暂的MCAO治疗75分钟,然后再灌注(3或24小时)。我们通过适当的方法测量了大脑中促炎性细胞因子(IL-1β,TNF-α,IL-6),ICAM-1,IL-10和pSTAT-3的表达。我们还研究了缺血和再灌注(I / R)后白细胞(FACS)中的细胞毒性T细胞亚群以及脑中炎症细胞的活化和募集(使用髓过氧化物酶活性测定)。使用免疫荧光法分别分析了大脑同侧半球中的凋亡(TUNEL)以及Bcl-xL-和Foxp3-(Treg标记)阳性细胞。结果我们的结果表明,闭塞后3小时再灌注会增加同侧半球中促炎性细胞因子和ICAM-1基因的表达,霍桑预处理显着降低了这些水平(p≤0.01)。此外,这种预处理能够在再灌注24小时后增加大脑中的IL-10水平和Foxp3阳性细胞。用Hawthorn预处理,在再灌注24小时后,运载体大鼠中细胞毒性T细胞群体的增加减少了至少40%。另外,预处理的脑中炎性细胞活化和浸润减少。 I / R后,山楂预处理可提高大脑中pSTAT-3的水平。我们还观察到Bcl-xL阳性细胞的增加,与媒介物治疗的大脑相比,Bcl-xL阳性细胞的减少又可能影响了TUNEL阳性细胞的减少。结论总而言之,山楂提取物有助于减轻与I / R诱导的损伤相关的促炎性免疫反应,提高IL-10水平并增加脑中Foxp3阳性Treg,这可能有助于抑制活化的炎性细胞。通过影响大脑中的STAT-3磷酸化和Bcl-xL表达,这种治疗还可以使凋亡细胞的死亡最小化。两者合计,山楂提取物的免疫调节作用可能在此MCAO诱导的中风模型中观察到的神经保护中起关键作用。

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