Treatment of Parkinson's disease in Zebrafish model with a berberine derivative capable of crossing blood brain barrier, targeting mitochondria, and convenient for bioimaging experiments

小檗碱 神经保护 斑马鱼 药理学 MPTP公司 线粒体 帕金森病 生物碱 化学 多巴胺能 细胞生物学 生物化学 多巴胺 生物 神经科学 医学 病理 疾病 立体化学 基因
作者
Lizhen Wang,Wenlong Sheng,Zhaoshun Tan,Qingyu Ren,Rongchun Wang,Rostyslav Stoika,Xuedong Liu,Kechun Liu,Xueliang Shang,Meng Jin
出处
期刊:Comparative Biochemistry and Physiology C-toxicology & Pharmacology [Elsevier BV]
卷期号:249: 109151-109151 被引量:27
标识
DOI:10.1016/j.cbpc.2021.109151
摘要

Berberine is a famous alkaloid extracted from Berberis plants and has been widely used as medications and functional food additives. Recent studies reveal that berberine exhibits neuroprotective activity in animal models of Parkinson's disease (PD), the second most prevalent neurodegenerative disorders all over the world. However, the actual site of anti-PD action of berberine remains largely unknown. To this end, we employed a fluorescently labeled berberine derivative BBRP to investigate the subcellular localization and blood brain barrier (BBB) permeability in a cellular model of PD and zebrafish PD model. Biological investigations revealed that BBRP retained the neuroprotective activity of berberine against PD-like symptoms in PC12 cells and zebrafish, such as protecting 6-OHDA induced cell death, relieving MPTP induced PD-like behavior and increasing dopaminergic neuron loss in zebrafish. We also found that BBRP could readily penetrate BBB and function in the brain of zebrafish suffering from PD. Subcellular localization study indicated that BBRP could rapidly and specifically accumulate in mitochondria of PC12 cells when it exerted anti-PD effect. In addition, BBRP could suppress accumulation of Pink1 protein and inhibit the overexpression of LC3 protein in 6-OHDA damaged cells. All these results suggested that the potential site of action of berberine is mitochondria in the brain under the PD condition. Therefore, the findings described herein would be useful for further development of berberine as an anti-PD drug. • A fluorescently labeled berberine derivative BBRP exhibits higher neuroprotective activity than berberine. • BBRP can rapidly and specifically accumulate in mitochondria of PC12 cells when it exerted anti-PD effect. • BBRP can readily penetrate BBB and function in the brain of zebrafish suffering from PD.
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