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Inhibition of Amyloid Beta Aggregation and Deposition of Cistanche tubulosa Aqueous Extract

机译:抑制淀粉样蛋白β聚集和脊柱管含水提取物的沉积

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摘要

Cistanche tubulosa aqueous extract (CTE) is already used as a botanical prescription drug for treating dementia in China. Our previous studies reported that phenylethanoid glycosides of CTE have anti-Alzheimer’s disease (AD) activity by inhibiting amyloid β peptide (Aβ) aggregation and deposition. However, recent studies considered that the phenylethanoid glycosides may be metabolized by intestinal bacteria, because all analysis results showed that the bioavailability of phenylethanoid glycosides is extremely low. In this study we demonstrate how iron chelation plays a crucial role in the Aβ aggregation and deposition inhibition mechanism of phenylethanoid glycosides of CTE. In addition, we further proved phenylethanoid glycosides (1⁻3) could reach brain. Active CTE component and action mechanism confirmation will be a great help for product quality control and bioavailability studies in the future. At the same time, we provide a new analysis method useful in determining phenylethanoid glycosides (1⁻3) in plants, foods, blood, and tissues for chemical fingerprint and pharmacokinetic research.
机译:Cistanche Tubulosa含水提取物(CTE)已被用作治疗中国痴呆的植物处方药。我们以前的研究报道说,CTE的苯乙酸糖苷通过抑制淀粉样蛋白β肽(Aβ)聚集和沉积具有抗阿尔茨海默病(Ad)活性。然而,最近的研究认为,苯乙醇苷糖苷可以通过肠道核化代谢,因为所有分析结果表明,苯乙醇糖苷的生物利用度极低。在这项研究中,我们展示了铁螯合在CTE的苯基乙醇糖苷的Aβ聚集和沉积抑制机制中的作用是如何发挥至关重要的作用。此外,我们进一步证明了苯乙醇糖苷(1⁻3)可以达到脑。有源CTE组件和动作机制确认将是未来产品质量控制和生物利用度研究的大大帮助。同时,我们提供了一种新的分析方法,可用于在化学指纹和药代动力学研究中确定植物,食品,血液和组织中的苯乙醇糖苷(1⁻3)。

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