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人参皂苷Rg1在阿尔茨海默病小鼠模型中的多面神经保护作用。

Multi-faced neuroprotective effects of Ginsenoside Rg1 in an Alzheimer mouse model.

作者信息

Fang Fang, Chen Xiaochun, Huang Tianwen, Lue Lih-Fen, Luddy John S, Yan Shirley Shidu

机构信息

Department of Surgery, Physicians & Surgeons College of Columbia University, New York, NY 10032, USA.

出版信息

Biochim Biophys Acta. 2012 Feb;1822(2):286-92. doi: 10.1016/j.bbadis.2011.10.004. Epub 2011 Oct 12.

Abstract

There has been no extensive characterization of the effects of Ginsenoside Rg1, a pharmacological active component purified from the nature product ginseng, in an Alzheimer's disease mouse model. The well-characterized transgenic Alzheimer disease (AD) mice over expressing amyloid precursor protein (APP)/Aβ (Tg mAPP) and nontransgenic (nonTg) littermates at age of 6 and 9 months were treated with Rg 1 for three months via intraperitoneal injection. Mice were then evaluated for changes in amyloid pathology, neuropathology and behavior. Tg mAPP treated with Rg1 showed a significant reduction of cerebral Aβ levels, reversal of certain neuropathological changes, and preservation of spatial learning and memory, as compared to vehicle-treated mice. Rg1 treatment inhibited activity of γ-secretase in both Tg mAPP mice and B103-APP cells, indicating the involvement of Rg1 in APP regulation pathway. Furthermore, administration of Rg1 enhanced PKA/CREB pathway activation in mAPP mice and in cultured cortical neurons exposed to Aβ or glutamate-mediated synaptic stress. Most importantly, the beneficial effects on attenuation of cerebral Aβ accumulation, improvement in neuropathological and behavioral changes can be extended to the aged mAPP mice, even to 12-13 months old mice that had extensive amyloid pathology and severe neuropathological and cognitive malfunction. These studies indicate that Rg1 has profound multi-faced and neuroprotective effects in an AD mouse model. Rg1 induces neuroprotection through ameliorating amyloid pathology, modulating APP process, improving cognition, and activating PKA/CREB signaling. These findings provide a new perspective for the treatment of AD and demonstrate potential for a new class of drugs for AD treatment.

摘要

从天然产物人参中纯化得到的药理活性成分人参皂苷Rg1在阿尔茨海默病小鼠模型中的作用尚未得到广泛表征。对6个月和9个月大的、已充分表征的过表达淀粉样前体蛋白(APP)/Aβ的转基因阿尔茨海默病(AD)小鼠(Tg mAPP)及其非转基因(nonTg)同窝小鼠进行为期三个月的腹腔注射Rg1治疗。然后评估小鼠在淀粉样病理、神经病理和行为方面的变化。与溶剂处理的小鼠相比,用Rg1处理的Tg mAPP小鼠脑内Aβ水平显著降低,某些神经病理变化得到逆转,空间学习和记忆得以保留。Rg1处理抑制了Tg mAPP小鼠和B103-APP细胞中γ-分泌酶的活性,表明Rg1参与了APP调节途径。此外,给予Rg1增强了mAPP小鼠以及暴露于Aβ或谷氨酸介导的突触应激的培养皮质神经元中PKA/CREB途径的激活。最重要的是,对脑内Aβ积累的减轻、神经病理和行为变化的改善等有益作用可以扩展到老年mAPP小鼠,甚至是12 - 13个月大、具有广泛淀粉样病理以及严重神经病理和认知功能障碍的小鼠。这些研究表明RgI在AD小鼠模型中具有深刻的多方面神经保护作用=Rg1通过改善淀粉样病理、调节APP加工过程、改善认知以及激活PKA/CREB信号传导来诱导神经保护。这些发现为AD的治疗提供了新视角,并证明了一类新型AD治疗药物的潜力。

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本文引用的文献

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