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基于壳聚糖接枝多巴胺的胶束作为多功能纳米药物用于帕金森病鼻内给药治疗的合成与表征

Synthesis and characterization of chitosan-grafted-dopamine based micelles as multifunctional nanomedicines for Parkinson's disease treatment by intranasal administration.

作者信息

Trapani Adriana, Carbone Annalucia, Gioia Sante Di, Fracchiolla Giuseppe, Soccio Piera, Perna Filippo Maria, Quivelli Andrea Francesca, Suranna Gian Paolo, Grisorio Roberto, Porto Chiara Lo, Conelli Daniele, Colangelo Giuditta, Conese Massimo

机构信息

Department of Pharmacy-Drug Sciences, University of Bari Aldo Moro, via E. Orabona, 4-70125, Bari, Italy.

Department of Clinical and Experimental Medicine, University of Foggia, 71122, Foggia, Italy.

出版信息

Drug Deliv Transl Res. 2025 Sep 1. doi: 10.1007/s13346-025-01963-0.

DOI:10.1007/s13346-025-01963-0
PMID:40890327
Abstract

The main aim of this work was to synthesize new chitosan amphiphilic derivatives able to self-assembly encapsulating substances acting at different target sites implicated in Parkinson disease (PD). For this purpose, O-carboxymethyl-chitosan (O-CMCS) was grafted with dopamine (DA) exploiting a carbodiimide mediated coupling reaction using different polymer/DA weight ratios. The structural characterization of the resulting O-CMCS-g-DA conjugates was carried out by spectral (i.e., ì FT-IR, H-NMR spectroscopy) and potentiometric titrations. The physicochemical characterization of these conjugates was performed by thermal analysis, scanning electron microscopy coupled with energy dispersive X-ray spectroscopy. The in vitro DA release was carried out in simulated nasal fluid showing in any case a sustained release of the neurotransmitter. The amphiphilic O-CMCS-g-DA conjugate at highest substitution degree was allowed to form micelles using the dialysis method. The Critical Micellar Concentration of such micelles was determined by the conductometric method and resulted of 1 × 10 mg/mL Quercetin (QUE), selected as hydrophobic antioxidant model drug, was encapsulated into the core of these micelles with an efficiency of 18%. From a biological point of view, none of the O-CMCS-g-DA conjugates was cytotoxic against the target neuronal SH-SY5Y cells. Moreover, all the O-CMCS-g-DA conjugates were able to modulate neuroinflammation as demonstrated by mRNA expression level analysis. Therefore, these O-CMCS-g-DA based micelles showed a great potential as multifunctional nanomedicines for brain delivery by intranasal route of a lipophilic antioxidant involved in the oxidative stress together with the neurotransmitter DA exploiting a delivery system with modulating properties of neuroinflammation.

摘要

这项工作的主要目的是合成新的壳聚糖两亲性衍生物,这些衍生物能够自组装以包封作用于帕金森病(PD)相关不同靶点的物质。为此,利用碳二亚胺介导的偶联反应,以不同的聚合物/多巴胺(DA)重量比将O-羧甲基壳聚糖(O-CMCS)与多巴胺进行接枝。通过光谱法(即傅里叶变换红外光谱、核磁共振氢谱)和电位滴定法对所得的O-CMCS-g-DA共轭物进行结构表征。通过热分析、扫描电子显微镜结合能量色散X射线光谱对这些共轭物进行物理化学表征。在模拟鼻液中进行体外DA释放,结果表明在任何情况下神经递质均为持续释放。使用透析法使最高取代度的两亲性O-CMCS-g-DA共轭物形成胶束。通过电导法测定此类胶束的临界胶束浓度,结果为1×10 mg/mL。槲皮素(QUE)作为疏水性抗氧化模型药物,以18%的效率被包封在这些胶束的核心中。从生物学角度来看,所有O-CMCS-g-DA共轭物对目标神经元SH-SY5Y细胞均无细胞毒性。此外,如mRNA表达水平分析所示,所有O-CMCS-g-DA共轭物均能够调节神经炎症。因此,这些基于O-CMCS-g-DA的胶束作为多功能纳米药物具有巨大潜力,可通过鼻内途径递送参与氧化应激的亲脂性抗氧化剂以及神经递质DA,并利用具有调节神经炎症特性的递送系统实现脑内递送。

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本文引用的文献

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Recent advances in nanotechnology for Parkinson's disease: diagnosis, treatment, and future perspectives.帕金森病纳米技术的最新进展:诊断、治疗及未来展望。
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