Molecularly imprinted cyclodextrin nanosponges for the controlled delivery of L-DOPA: perspectives for the treatment of Parkinson’s disease

化学 前药 多巴胺 环糊精 分子印迹聚合物 水溶液 分子印迹 药物输送 傅里叶变换红外光谱 核化学 动力学 药理学 组合化学 色谱法 选择性 有机化学 生物化学 催化作用 化学工程 医学 内分泌学 工程类 物理 量子力学
作者
Francesco Trotta,Fabrizio Caldera,Roberta Cavalli,Marco Soster,Chiara Riedo,Miriam Biasizzo,Gloria Uccello‐Barretta,Federica Balzano,Valentina Brunella
出处
期刊:Expert Opinion on Drug Delivery [Taylor & Francis]
卷期号:13 (12): 1671-1680 被引量:85
标识
DOI:10.1080/17425247.2017.1248398
摘要

L-DOPA is an amino acid precursor to the neurotransmitter dopamine that is extensively used as a prodrug for the treatment of Parkinson's disease. However, L-DOPA is an unstable compound: when exposed to light or added to aqueous solutions, it may degrade, compromising its therapeutic properties.In this work, a new type of drug-loaded cyclodextrin-based nanosponge, obtained using molecular imprinting, is described for the prolonged and controlled release of L-DOPA. The molecularly imprinted nanosponges (MIP-NSs) were synthesized by cross-linking β-cyclodextrin with 1,1'-carbonyldiimidazole in DMF in the presence of L-DOPA as a template molecule. TGA, DSC and FTIR analyses were performed to characterize the interactions between L-DOPA and the two nanosponge structures. Quantitative NMR spectroscopy was used to determine the amount and the affinity of L-DOPA entrapped in the nanosponges. The in vitro L-DOPA release kinetics from the NSs were quantitatively determined by HPLC analysis.The MIP-NSs show a slower and more prolonged release profile than the non-imprinted nanosponges. No degradation of the L-DOPA hosted in the MIP-NSs was observed after long-term storage at room temperature.The MIP-NSs are a promising alternative for the storage and controlled delivery of L-DOPA.
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