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壳聚糖载氟康唑载溶菌酶纳米粒增强三维尿路上皮细胞模型生物膜清除作用。

Enhanced clearing of biofilms on a 3D urothelial cell model using lysozyme-functionalized fluconazole-loaded shellac nanoparticles.

机构信息

Department of Chemistry, University of Hull, Cottingham Road, Hull, HU67RX, UK.

Department of Biomedical Sciences, University of Hull, Hull, HU67RX, UK.

出版信息

Biomater Sci. 2021 Oct 12;9(20):6927-6939. doi: 10.1039/d1bm01035b.

DOI:10.1039/d1bm01035b
PMID:34528638
Abstract

urinary tract biofilms are increasingly witnessed in nosocomial infections due to reduced immunity of patients and the hospital ecosystem. The indwelling devices utilized to support patients with urethral diseases that connect the unsterilized external environment with the internal environment of the patient are another significant source of urinary tract biofilm infections. Recently, nanoparticle (NP)-associated therapeutics have gained traction in a number of areas, including fighting antibiotic-resistant bacterial biofilm infection. However, most studies on nanotherapeutic delivery have only been carried out in laboratory settings rather than in clinical trials due to the lack of precise and models for testing their efficiency. Here we develop a novel biofilm-infected 3D human urothelial cell culture model to test the efficiency of nanoparticle (NP)-based antifungal therapeutics. The NPs were designed based on shellac cores, loaded with fluconazole and coated with the cationic enzyme lysozyme. Our formulation of 0.2 wt% lysozyme-coated 0.02 wt% fluconazole-loaded 0.2 wt% shellac NPs, sterically stabilised by 0.25 wt% poloxamer 407, showed an enhanced efficiency in removing biofilms formed on 3D layer of urothelial cell clusteroids. The NP formulation exhibited low toxicity to urothelial cells. This study provides a reliable model for urinary tract biofilm infections, which could potentially replace animal models in the testing of such antifungal nanotechnologies. The reproducibility and availability of a well-defined biofilm-infected 3D urothelial cell culture model give valuable insights into the formation and clearing of fungal biofilms and could accelerate the clinical use of antifungal nanotherapeutics.

摘要

尿路生物膜由于患者免疫力下降和医院生态系统的原因,在医院感染中越来越常见。用于支持尿道疾病患者的留置装置将未消毒的外部环境与患者的内部环境连接起来,这是尿路生物膜感染的另一个重要来源。最近,纳米颗粒(NP)相关治疗在许多领域引起了关注,包括对抗抗生素耐药细菌生物膜感染。然而,由于缺乏精确和可靠的模型来测试其效率,大多数纳米治疗药物输送的研究仅在实验室环境中进行,而不是在临床试验中进行。在这里,我们开发了一种新型的生物膜感染的 3D 人尿路上皮细胞培养模型,以测试基于 NP 的抗真菌治疗的效率。NP 是基于紫胶核设计的,负载氟康唑,并涂有阳离子酶溶菌酶。我们的配方为 0.2wt%溶菌酶涂覆的 0.02wt%氟康唑负载的 0.2wt%紫胶 NP,由 0.25wt%泊洛沙姆 407 稳定,在去除在尿路上皮细胞集落 3D 层上形成的生物膜方面表现出更高的效率。NP 配方对尿路上皮细胞表现出低毒性。这项研究提供了一种可靠的尿路生物膜感染模型,它有可能取代动物模型来测试这种抗真菌纳米技术。可重复性和生物膜感染的 3D 尿路上皮细胞培养模型的可用性为真菌生物膜的形成和清除提供了有价值的见解,并可以加速抗真菌纳米治疗的临床应用。

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