探索新型三元共聚物纳米粒子系统,防止酒精引起的剂量倾倒。

IF 4.5 2区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL
Kuan Chen, Hao Han R Chang, Jamie Lugtu-Pe, Yuan Gao, Fuh-Ching Liu, Anil Kane, Xiao Yu Wu
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引用次数: 0

摘要

酒精诱导的剂量倾倒(AIDD)仍然是阿片类药物等高效力药物控制给药过程中面临的一个严峻挑战,需要进行广泛的研究并找到创新的解决方案。目前的技术依赖于瓜尔胶和海藻酸钠等不溶于乙醇的辅料来抵消疏水性聚合物辅料在乙醇中增加的溶解度。然而,这些辅料存在一些缺点,如包衣分散体粘度高、溶液温度高、凝胶化速度快、成膜不均匀等。在这项研究中,我们探索了交联三元共聚物纳米粒子(TPN)作为抗酒精辅料在乙基纤维素(EC)水不溶控释膜中的应用,以预防艾滋。在此,我们采用中心复合设计(CCD)优化了 TPN 的组成,以尽量减少 TPN-EC 薄膜在 20% 乙醇存在下的溶胀和重量损失。优化后的 TPN 对涂层分散体的粘度影响微乎其微,而瓜尔豆胶则使粘度增加了 76 倍。在含有 0% 或 40% v/v 乙醇的 pH 值为 1.2 的介质中进行的渗透性研究表明,阳离子药物(盐酸普萘洛尔、盐酸地尔硫卓和盐酸纳洛酮(阿片受体结合模型药物))的渗透率(P40%/P0%)明显低于非离子药物(茶碱和水杨酸)。傅立叶变换红外分析表明,在乙醇存在的情况下,TPN 与阳离子药物之间的离子氢键增加。这些结果表明,药物-聚合物-溶剂之间的相互作用在 TPN-EC 薄膜不依赖酒精的药物渗透性中发挥了重要作用。利用 TPN-EC 系统改变药物渗透性的能力,阳离子药物在水乙醇介质中的释放似乎受到了抑制,这表明这是一种很有前景的抗酒精新机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Exploration of a Novel Terpolymer Nanoparticle System for the Prevention of Alcohol-Induced Dose Dumping.

Alcohol-induced dose dumping (AIDD) remains a serious challenge in the controlled delivery of high potency drugs, such as opioids, which requires extensive investigation and innovative solutions. Current technologies rely on ethanol-insoluble excipients, such as guar gum and sodium alginate, to counteract the increased solubility of hydrophobic polymeric excipients in ethanol. However, these excipients pose several shortcomings, such as high viscosity of coating dispersion, high solution temperature, rapid gelation, and heterogeneity of resulted film. In this work, we explored the application of a cross-linked terpolymer nanoparticle (TPN) as an alcohol-resistant excipient in a water-insoluble controlled release film of ethylcellulose (EC) for the prevention of AIDD. Herein, we optimized the composition of TPN using a central composite design (CCD) to minimize swelling and weight loss of TPN-EC film in the presence of 20% ethanol. The optimized TPN showed a negligible effect on the viscosity of the coating dispersion, while guar gum increased the viscosity by 76-fold. Permeability studies in a pH 1.2 media containing 0% or 40% v/v ethanol revealed that cationic drugs (propranolol HCl, diltiazem HCl, and naloxone HCl (an opioid receptor-binding model drug)) exhibited significantly lower permeability ratios (P40%/P0%) than un-ionized drugs (theophylline and salicylic acid). FTIR analysis indicated an increase in ionic hydrogen bonding between TPN and the cationic drug in the presence of ethanol. These results suggest that drug-polymer-solvent interactions play an important role in alcohol-independent drug permeability through the TPN-EC film. By leveraging the drug permeability altering capability of the TPN-EC system, the release of cationic drugs in hydroethanolic media appeared to be suppressed, suggesting a promising new mechanism of alcohol resistance.

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来源期刊
Molecular Pharmaceutics
Molecular Pharmaceutics 医学-药学
CiteScore
8.00
自引率
6.10%
发文量
391
审稿时长
2 months
期刊介绍: Molecular Pharmaceutics publishes the results of original research that contributes significantly to the molecular mechanistic understanding of drug delivery and drug delivery systems. The journal encourages contributions describing research at the interface of drug discovery and drug development. Scientific areas within the scope of the journal include physical and pharmaceutical chemistry, biochemistry and biophysics, molecular and cellular biology, and polymer and materials science as they relate to drug and drug delivery system efficacy. Mechanistic Drug Delivery and Drug Targeting research on modulating activity and efficacy of a drug or drug product is within the scope of Molecular Pharmaceutics. Theoretical and experimental peer-reviewed research articles, communications, reviews, and perspectives are welcomed.
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