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负载金诺芬纳米颗粒的复合热响应水凝胶用于阴道毛滴虫感染的局部治疗。

Composite thermoresponsive hydrogel with auranofin-loaded nanoparticles for topical treatment of vaginal trichomonad infection.

作者信息

Zhang Yue, Miyamoto Yukiko, Ihara Sozaburo, Yang Justin Z, Zuill Douglas E, Angsantikul Pavimol, Zhang Qiangzhe, Gao Weiwei, Zhang Liangfang, Eckmann Lars

机构信息

Department of NanoEngineering and Moores Cancer Center, University of California San Diego, La Jolla, California 92093, USA.

Department of Medicine, University of California San Diego, La Jolla, California 92093, USA.

出版信息

Adv Ther (Weinh). 2019 Dec;2(12). doi: 10.1002/adtp.201900157. Epub 2019 Oct 30.

Abstract

is responsible for the most common non-viral sexually-transmitted disease worldwide. Standard treatment is with oral nitro-heterocyclic compounds, metronidazole or tinidazole, but resistance to these drugs is emerging and adverse effects can be problematic. Topical treatment offers potential benefits for increasing local drug concentrations and efficacy, while reducing systemic drug exposure, but no topical strategies are currently approved for trichomoniasis. The anti-rheumatic drug, auranofin (AF), was recently discovered to have significant trichomonacidal activity, but has a long plasma half-life and significant adverse effects. Here, we used this drug as a model to develop a novel topical formulation composed of AF-loaded nanoparticles (NP) embedded in a thermoresponsive hydrogel for intravaginal administration. The AF-NP composite gel showed sustained drug release for at least 12 h, and underwent sol-gel transition with increased viscoelasticity within a minute. Intravaginal administration in mice showed excellent NP retention for >6 h and markedly increased local AF levels, but reduced plasma and liver levels compared to oral treatment with a much higher dose. Furthermore, intravaginal AF-NP gel greatly outperformed oral AF in eliminating vaginal trichomonad infection in mice, while causing no systemic or local toxicity. These results show the potential of the AF-NP hydrogel formulation for effective topical therapy of vaginal infections.

摘要

在全球范围内引发最常见的非病毒性传播疾病。标准治疗方法是使用口服硝基杂环化合物、甲硝唑或替硝唑,但对这些药物的耐药性正在出现,且不良反应可能成为问题。局部治疗在提高局部药物浓度和疗效的同时减少全身药物暴露方面具有潜在益处,但目前尚无用于滴虫病的局部治疗策略获批。抗风湿药物金诺芬(AF)最近被发现具有显著的杀滴虫活性,但血浆半衰期长且有明显不良反应。在此,我们以该药物为模型,开发了一种新型局部制剂,由负载AF的纳米颗粒(NP)嵌入热响应水凝胶组成,用于阴道给药。AF-NP复合凝胶显示药物持续释放至少12小时,并在一分钟内发生溶胶-凝胶转变,粘弹性增加。小鼠阴道给药显示NP在体内保留超过6小时,局部AF水平显著升高,但与高得多剂量的口服治疗相比,血浆和肝脏中的水平降低。此外,阴道内给予AF-NP凝胶在消除小鼠阴道滴虫感染方面大大优于口服AF药物,同时未引起全身或局部毒性。这些结果表明AF-NP水凝胶制剂在有效局部治疗阴道感染方面的潜力。

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