转录组分析揭示了芒果苷在斑马鱼体内的抗帕金森病活性。

Fengqing Qin, Ming Zhang, Pei Wang, Ziru Dai, Xi Li, Dongliang Li, Lijun Jing, Cen Qi, Heliang Fan, Mei Qin, Ying Li, Likun Huang, Tianci Wang
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摘要

随着全球人口的老龄化,帕金森病(PD)的发病率持续上升,给社会和经济造成了巨大负担。多酚类生物活性化合物芒果苷(Mangiferin,MGF)已被证明在帕金森病的预防和治疗中发挥作用。本研究通过转录组分析,研究了 MGF 在 MPTP 诱导的斑马鱼脑退化症模型中的神经保护作用。首先,使用不同的 MPTP 和 MGF 组合确定了建模的最佳浓度。然后将斑马鱼分为对照组、MPTP 处理组和 MGF 联合处理组。随后的评估包括孵化率、死亡率、生长发育状况、自发运动能力以及 SOD、CAT 酶活性和 GSH 水平的测量。最后,通过转录组测序评估了 MGF 对斑马鱼帕金森病模型的疗效。结果表明,MPTP 治疗可诱导斑马鱼出现与帕金森病相关的症状,而 MGF 治疗可显著提高帕金森病模型斑马鱼的运动能力和存活率,有效降低氧化应激,改善帕金森病症状。转录组测序进一步发现,MGF可通过调节包括lrrk2、vps35、atp13a、dnajc6和uchl1在内的关键基因的表达,减轻帕金森病斑马鱼体内与线粒体相关的氧化应激。差异基因表达分析表明,这些基因主要参与重要的信号通路,如神经活性配体-受体相互作用和钙信号通路。总之,我们的研究提供了有力的科学证据,支持 MGF 通过保护线粒体稳态和阐明其作用机制成为治疗帕金森病的潜在候选药物。
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Transcriptome analysis reveals the anti-Parkinson's activity of Mangiferin in zebrafish.

As the global population ages, the incidence of Parkinson's Disease (PD) continues to rise, imposing significant social and economic burdens. Mangiferin (MGF), a polyphenolic, bioactive compound has been shown to play a role in the prevention and treatment of PD. This study investigates the neuroprotective effects of MGF in an MPTP-induced zebrafish model of PD through transcriptome analysis. Initially, optimal concentrations for modeling were determined using various MPTP and MGF combinations. The zebrafish were then divided into control, MPTP-treated, and MGF co-treated groups. Subsequent evaluations included hatching rates, mortality rates, growth and development conditions, spontaneous motor abilities, as well as measurements of enzymatic activities of SOD, CAT, and levels of GSH. Ultimately, the therapeutic efficacy of MGF on the PD model in zebrafish was assessed through transcriptome sequencing. The results demonstrated that MPTP treatment induced PD-associated symptoms in zebrafish, while MGF treatment significantly improved the motor abilities and survival rates of the PD model zebrafish, effectively reducing oxidative stress and ameliorating PD symptoms. Transcriptome sequencing further revealed that MGF may mitigate mitochondrial-related oxidative stress in PD zebrafish by modulating the expression of critical genes including lrrk2, vps35, atp13a, dnajc6, and uchl1. Differential gene expression analysis indicated that these genes are primarily involved in vital signaling pathways, such as neuroactive ligand-receptor interaction, and the calcium signaling pathway. In summary, our study provides robust scientific evidence supporting MGF as a potential therapeutic candidate for PD by preserving mitochondrial homeostasis and elucidating its mechanisms of action.

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Corrigendum to "Sialogogic effects through olfactory stimulation with mastic resin and α-pinene volatiles in vivo" [Biomed. Pharmacother. 168 (2023) 1-9]. Corrigendum to "Dual regulatory effects of neferine on amyloid-β and tau aggregation studied by in silico, in vitro, and lab-on-a-chip technology" [Biomed. Pharmacother. 172 (2024) 1-14/116226]. Corrigendum to "Celastrol reduces IL-1β induced matrix catabolism, oxidative stress and inflammation in human nucleus pulposus cells and attenuates rat intervertebral disc degeneration in vivo" [Biomed. Pharmacother., 91 (2017) 208-219]. Corrigendum to "Mechanism of chromium-induced toxicity in lungs, liver, and kidney and their ameliorative agents" [Biomed. Pharmacother. 151, July 2022, 113119]. Corrigendum to Pro-cognitive effects of dual tacrine derivatives acting as cholinesterase inhibitors and NMDA receptor antagonists "Biomed. Pharmacother. 176 (2024) 116821".
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