Chrysin loaded Nanostructured lipid carrier (NLC) drug delivery system: Harnessing neuroprotective effects in the management of Alzheimer’s Disease

白杨素 神经保护 药理学 纳米载体 药物输送 生物利用度 背景(考古学) 药品 化学 医学 纳米技术 抗氧化剂 材料科学 生物化学 生物 类黄酮 古生物学
作者
Nikhil Khandale,Devendra Birla,Bushra Bashir,Sachin Kumar Singh,Sukriti Vishwas,Monica Gulati,Kamal Dua
出处
期刊:Alzheimers & Dementia [Wiley]
卷期号:20 (S6) 被引量:1
标识
DOI:10.1002/alz.088755
摘要

Abstract Background Alzheimer’s Disease (AD) poses a substantial global health burden, necessitating innovative therapeutic strategies. This study investigates the neuroprotective potential of a chrysin‐loaded Nanostructured Lipid Carrier (NLC) drug delivery system in AD management. Employing the high‐pressure homogenization method, chrysin‐loaded NLCs were meticulously formulated to optimize drug delivery efficiency. The research explores the multifaceted neuroprotective effects of chrysin, a naturally occurring flavonoid, within the context of AD pathology. The intricate mechanisms of action underlying the chrysin‐loaded NLCs are elucidated, shedding light on their potential to modulate key pathways implicated in AD progression. This study advances our understanding of tailored drug delivery systems, specifically highlighting the therapeutic promise of chrysin‐loaded NLCs for the nuanced management of Alzheimer’s Disease. Method To overcome these challenges, a Nanostructured lipid carrier (NLC) for Chrysin was devised, employing quality by design (QbD) based Box‐Behnken design (BBD). NLC offers numerous advantages, encompassing increased drug loading, facile preparation, exceptional stability, as well as enhanced bioavailability and permeability across the blood‐brain barrier. Result The optimized Chrysin‐loaded NLC formulation exhibited Particle Size, PDI, zeta potential, and drug loading as 66.45nm, 0.19, ‐22mV, and 98% respectively. The formulation was found to be stable after six months in accelerated stability studies. The formulation underwent various pharmacodynamic studies. Pharmacodynamic studies assessed cognitive and motor functions in rats, revealing significant improvements in cognition with both low and high doses respectively. Additionally, the biochemical investigations revealed that the Chrysin‐loaded NLCs effectively decreased the levels AChE enzyme, amyloid β, oxidative stress, and neuroinflammation. Conclusion This study explores Chrysin‐loaded NLCs as a solution for challenges in Alzheimer’s Disease (AD) treatment. The optimized formulation overcomes Chrysin’s solubility issues, demonstrating improved bioavailability and permeability. Chrysin‐loaded NLCs hold promise as a neuroprotective for AD.
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