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积雪草苷通过调控 mTOR 信号通路减少自噬,改善痴呆大鼠的记忆。

Asiaticoside reduces autophagy and improves memory in a rat model of dementia through mTOR signaling pathway regulation.

机构信息

Department of Neurology, Aerospace Center Hospital, Peking University Aerospace School of Clinical Medicine, Beijing 100049, P.R. China.

Department of Neurosurgery, Dongying District People's Hospital of Dongying City, Dongying, Shandong 257000, P.R. China.

出版信息

Mol Med Rep. 2021 Sep;24(3). doi: 10.3892/mmr.2021.12284. Epub 2021 Jul 19.

Abstract

Vascular dementia (VD) is one of the leading causes of neurological disorder following Alzheimer's disease. The present study evaluated the possible role of asiaticoside in the treatment of rats with VD and its inhibitory effects on autophagy in hippocampal tissues. Double ligation was used for permanent occlusion of the arteries, and spatial memory was assessed using the T‑maze test. Western blotting was used for determination of protein expression levels and H&E staining for histological analysis. Treatment of rats with VD with asiaticoside significantly alleviated the impairment in spontaneously altered behaviors and significantly reduced escape latency. VD mediated a decrease in distance travelled, swim time and number of platform crossings, whereas this was alleviated by asiaticoside. Furthermore, VD‑mediated hippocampal tissue damage was significantly alleviated by asiaticoside treatment (P<0.05), and asiaticoside alleviated formation of autophagosomes and markedly suppressed the number of primary lysosomes. In asiaticoside‑treated rats, VD‑mediated increases in Beclin 1 and microtubule‑associated protein light chain 3 (LC3) II expression in the hippocampal tissues were alleviated. Asiaticoside treatment also prevented suppression of mammalian target of rapamycin (mTOR) phosphorylation in VD rat hippocampal tissues. Notably, the rapamycin‑mediated suppression of phosphorylated‑mTOR, and elevation of Beclin 1 and LC3II expression in the rat hippocampus could not be alleviated by asiaticoside treatment. In conclusion, asiaticoside effectively prevented cerebral ischemia‑mediated cognitive impairment and neuronal damage in the rats. Moreover, autophagy was inhibited and the mTOR pathway was activated in rats with cerebral ischemia by asiaticoside treatment. Therefore, asiaticoside may warrant further study as a therapeutic agent for the treatment of dementia.

摘要

血管性痴呆(VD)是继阿尔茨海默病之后导致神经功能障碍的主要原因之一。本研究评估了积雪草苷治疗 VD 大鼠的可能作用及其对海马组织自噬的抑制作用。采用双重结扎法对动脉进行永久性闭塞,采用 T 迷宫试验评估空间记忆。采用 Western blot 法测定蛋白表达水平,H&E 染色进行组织学分析。用积雪草苷治疗 VD 大鼠可显著减轻自发行为改变受损,并显著降低逃避潜伏期。VD 介导的大鼠行进距离、游泳时间和平台穿越次数减少,而积雪草苷可减轻这种情况。此外,积雪草苷治疗可显著减轻 VD 介导的海马组织损伤(P<0.05),并减轻自噬体的形成,显著抑制初级溶酶体的数量。在积雪草苷治疗的大鼠中,VD 介导的海马组织中 Beclin 1 和微管相关蛋白轻链 3(LC3)II 表达的增加得到缓解。积雪草苷治疗还可防止 VD 大鼠海马组织中哺乳动物雷帕霉素靶蛋白(mTOR)磷酸化的抑制。值得注意的是,积雪草苷不能缓解雷帕霉素对大鼠海马组织中磷酸化 mTOR、Beclin 1 和 LC3II 表达的抑制作用。综上所述,积雪草苷可有效预防大鼠脑缺血介导的认知障碍和神经元损伤。此外,积雪草苷治疗可抑制自噬并激活缺血性大鼠的 mTOR 通路。因此,积雪草苷可能值得进一步研究作为治疗痴呆的药物。

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