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基于黏附性聚多巴胺的光热杂化水凝胶用于按需递送利多卡因、有效抗菌和延长局部长效镇痛。

Adhesive polydopamine-based photothermal hybrid hydrogel for on-demand lidocaine delivery, effective anti-bacteria, and prolonged local long-lasting analgesia.

机构信息

Department of Anesthesiology, First Affiliated Hospital, Sun Yat-sen University, Guangzhou 510080, China.

School of Chemical Engineering and Light Industry, Guangdong University of Technology, Guangzhou 510006, China.

出版信息

Int J Biol Macromol. 2024 Feb;259(Pt 2):129266. doi: 10.1016/j.ijbiomac.2024.129266. Epub 2024 Jan 8.

DOI:10.1016/j.ijbiomac.2024.129266
PMID:38199532
Abstract

Considering the astonishing prevalence of localized pain affecting billions of patients worldwide, the development of advanced analgesic formulations or delivery systems to achieve clinical applicability is of great significance. In this study, an integrated PDA-based LiH@PDA@Ag@PAA@Gelatin system was designed for sustained delivery of lidocaine hydrochloride (LiH). By optimizing the preparation process and formulation of the hydrogel, the hydrogel exhibited superior mechanical properties, reversibility, adhesion strength, and self-healing attributes. Moreover, PDA@Ag nanoparticles were evenly dispersed within the hydrogel, and the optimized PDA@Ag@PAA@Gelatin showed a higher photothermal conversion efficiency than that of pure PDA. Importantly, LiH@PDA@Ag@PAA@Gelatin could effectively capture and eradicate bacteria through the synergistic interaction between near-infrared (NIR), PDA, Ag and LiH. In vitro and in vivo tests demonstrated that LiH@PDA@Ag@PAA@Gelatin exhibited higher drug delivery efficiency compared to commercial lidocaine patches. By evaluating the mechanical pain withdrawal threshold of the spared nerve injury (SNI) model in rats, it was proven that LiH@PDA@Ag@PAA@Gelatin enhanced and prolonged the analgesic effect of LiH. Furthermore, LiH@PDA@Ag@PAA@Gelatin induced by NIR possessed excellent on-demand photothermal analgesic ability. Therefore, this study develops a convenient method for preparing localized analgesic hydrogel patches, providing an important step towards advancing PDA-based on-demand pain relief applications.

摘要

考虑到影响全球数十亿患者的局部疼痛惊人的普遍性,开发先进的镇痛制剂或输送系统以实现临床应用具有重要意义。在这项研究中,设计了一种基于 PDA 的 LiH@PDA@Ag@PAA@Gelatin 系统,用于盐酸利多卡因(LiH)的持续释放。通过优化水凝胶的制备工艺和配方,该水凝胶表现出优异的机械性能、可逆性、粘附强度和自修复特性。此外,PDA@Ag 纳米颗粒均匀分散在水凝胶中,优化后的 PDA@Ag@PAA@Gelatin 比纯 PDA 具有更高的光热转换效率。重要的是,LiH@PDA@Ag@PAA@Gelatin 可以通过近红外(NIR)、PDA、Ag 和 LiH 的协同作用有效捕获和消除细菌。体外和体内实验表明,与商业利多卡因贴剂相比,LiH@PDA@Ag@PAA@Gelatin 具有更高的药物传递效率。通过评估大鼠 spared 神经损伤(SNI)模型的机械疼痛回避阈值,证明 LiH@PDA@Ag@PAA@Gelatin 增强并延长了 LiH 的镇痛作用。此外,LiH@PDA@Ag@PAA@Gelatin 经 NIR 诱导具有出色的按需光热镇痛能力。因此,本研究开发了一种制备局部镇痛水凝胶贴片的简便方法,为推进基于 PDA 的按需止痛应用迈出了重要一步。

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