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首页> 外文期刊>Pharmacognosy Research >Targeted delivery of curcumin using MgONPs and solid lipid nanoparticles: Attenuates aluminum.induced neurotoxicity in albino rats
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Targeted delivery of curcumin using MgONPs and solid lipid nanoparticles: Attenuates aluminum.induced neurotoxicity in albino rats

机译:使用MgOnps和固体脂质纳米颗粒靶向姜黄素:衰减铝。在白化大鼠中诱导神经毒性

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Background: Aluminum is a potent environmental toxin and its increasing entry exposes human beings to its neurotoxicity. Objective: The authors investigated the efficacy of delivery systems (magnesium oxide nanoparticles [MgONPs] and solid lipid nanoparticles [SLNs]) for curcumin in protecting aluminum-induced neurotoxicity in albino rats. Materials and Methods: Albino rats were divided into six groups (n = 6), Group I served as control; Group II Al treated; Group III curcumin loaded MgONPs (CuMgONPs); Group IV Al CuMgONPs; Group V curcumin loaded SLNs (CuSLNs); Group VI Al CuSLNs. After the treatment period, i.e., 30 days the animals were sacrificed and biochemical tests were performed to assess the cholinergic damage followed by histological observation of brain regions (cerebral cortex and cerebellum). Results: In cholinergic analyses, it was observed that aluminum-induced alterations in ACh and acetylcholine esterase were reversed with concomitant administration of CuMgONPs and CuSLNs. The therapeutic potential of CuMgONPs and CuSLNs was also observed in histological analyses of brain regions treated with aluminum. Among these two drug delivery systems, CuSLNs administration was found to be more potential compared to the CuMgONPs in treating aluminum induced neurotoxicity. Conclusions: By using drug delivery systems, MgONPs and SLNs, the problem of low bioavailability of curcumin can be controlled. This will be a promising agent to treat neurodegenerative disorders such as Alzheimer's disease with the potentiality to cross the blood–brain barrier. However, CuSLNs has showed a more protective effect on altered cholinergic system and tissue damage compared to CuMgONPs.
机译:背景:铝是一种有效的环境毒素,其增加的进入将人类暴露于其神经毒性。目的:作者研究了递送系统(氧化镁纳米颗粒[MgOnps]和固体脂质纳米颗粒[SLNS])的疗效,用于保护铝诱导的白化大鼠神经毒性的姜黄素。材料和方法:将白性大鼠分为六组(n = 6),I基团用作控制; Al Al治疗;第三组姜黄素负载mgonps(Cumgonps);第IV组Al Cumgonps;组V姜黄素加载的SLNS(CUSLNS);组vi al cuslns。治疗期后,即,处死30天的动物并进行生物化学测试以评估胆碱能损伤,然后进行脑区组织学观察(脑皮层和小脑)。结果:在胆碱能分析中,观察到,伴随CumgOnps和Cuslns的铝诱导的ACH和乙酰胆碱酯酶的改变。在用铝处理的脑区域的组织学分析中也观察到Cumgonps和Cuslns的治疗潜力。在这两种药物递送系统中,与治疗铝诱导神经毒性的CUMGONP相比,发现CUSLNS给药更潜力。结论:通过使用药物递送系统,MGONP和SLN,可以控制姜黄素的低生物利用度问题。这将是一种有希望的药剂,用于治疗神经退行性疾病,如阿尔茨海默病,潜在能够穿过血脑屏障。然而,与Cumgonps相比,Cuslns对改变的胆碱能系统和组织损伤表现出更具保护作用。

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