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Icariin exerts estrogen-like activity in ameliorating EAE via mediating estrogen receptor β modulating HPA function and glucocorticoid receptor expression

机译:鹰嘴豆素通过介导雌激素受体β调节HPA功能和糖皮质激素受体表达在改善EAE中发挥类似雌激素的作用。

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摘要

Background: Estrogen exerts neuroprotective and anti-inflammatory effects in EAE and multiple sclerosis (MS), but its clinical application is hindered due to side effects and risk of tumor. Phytoestrogen structurally or functionally mimics estrogen with fewer side effects than endogenous estrogen. Icariin (ICA), an active component of Epimedium extracts, demonstrates estrogen-like neuroprotective effects. However, it is unclear whether ICA is effective in EAE and what are the underlying mechanisms. Objective: To determine the therapeutic effects of ICA in EAE and explore the possible mechanisms. Methods: C57BL/6 EAE mice were treated with Diethylstilbestrol, different dose of ICA and mid-dose ICA combined with ICI 182780. The clinical scores and serum Interleukin-17 (IL-17), Corticosterone (CORT) concentrations were then analyzed. Western blot were performed to investigate the expressions of glucocorticoid receptor (GR), estrogen receptor alpha (ERα) and ERβ in the cerebral white matter of EAE mice. Results: High dose ICA is equally effective in ameliorating neurological signs of EAE as estrogen. Estrogen and ICA has no effects on serum concentrations of IL-17 in EAE. While the CORT levels were decreased by ICA at mid or high doses, the expressions of GR, ERα and ERβ were up-regulated by estrogen or different doses of ICA in a dosedependent manner. Estrogen induced the elevation of ERα more markedly than ICA. In contrast, ICA at mid and high doses promoted ERβ more significantly than estrogen. Conclusion: ICA exerts estrogen-like activity in ameliorating EAE via mediating ERβ, modulating HPA function and up-regulating the expression of GR in cerebral white matter. ICA may be a promising therapeutic option for MS.
机译:背景:雌激素在EAE和多发性硬化症(MS)中发挥神经保护和抗炎作用,但由于副作用和肿瘤风险,其临床应用受到阻碍。与内源性雌激素相比,植物雌激素在结构或功能上模拟雌​​激素的副作用更少。淫羊(提取物的活性成分伊卡林(ICA)表现出类似雌激素的神经保护作用。但是,尚不清楚ICA在EAE中是否有效以及潜在的机制是什么。目的:确定ICA对EAE的治疗作用,并探讨可能的机制。方法:用己烯雌酚,不同剂量的ICA和中剂量ICA联合ICI 182780治疗C57BL / 6 EAE小鼠,并分析其临床评分和血清白细胞介素17(IL-17),皮质酮(CORT)浓度。进行了Western blot研究EAE小鼠脑白质中糖皮质激素受体(GR),雌激素受体α(ERα)和ERβ的表达。结果:高剂量ICA与雌激素一样,在改善EAE的神经系统症状方面同样有效。雌激素和ICA对EAE的血清IL-17没有影响。当中高剂量的ICA使CORT水平降低时,雌激素或不同剂量的ICA以剂量依赖性方式上调GR,ERα和ERβ的表达。雌激素比ICA更明显地诱导ERα升高。相反,中,高剂量ICA比雌激素更能促进ERβ。结论:ICA通过介导ERβ,调节HPA功能和上调GR在脑白质中的表达而具有雌激素样活性。 ICA可能是MS的有前途的治疗选择。

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