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气液界面肺部感染模型中的活性、吸入给药的可行性以及来自……的无细胞上清液对肺部感染的稳定性。 (注:原文中“from”后面似乎缺失了相关内容)

Activity in an air-liquid interface lung infection model, feasibility of inhaled delivery, and stability of cell-free supernatants from against pulmonary infections.

作者信息

Piras Anna Maria, Bianchi Marta, Bona Nicolò Della, Grassiri Brunella, Kaya Esingül, Bertacca Andrea, Migone Chiara, Maisetta Giuseppantonio, Esin Semih, Batoni Giovanna

机构信息

Department of Pharmacy, University of Pisa, Pisa, Italy.

Centre for Instrument Sharing of the University of Pisa (CISUP), Pisa, Italy.

出版信息

Front Microbiol. 2025 Aug 5;16:1630017. doi: 10.3389/fmicb.2025.1630017. eCollection 2025.

Abstract

OBJECTIVE

Given the increasing prevalence of multidrug-resistant pathogens and the diminishing efficacy of conventional antibiotics, this study explores the potential of probiotics or their metabolic products as alternative antimicrobial agents. Specifically, we investigated the antibacterial properties of cell-free supernatants (CFS) derived from the probiotic strain GG for the local treatment of lung infections.

METHODS

To simulate the human respiratory environment, we employed various models. The cytotoxicity and antibacterial activity of CFS were assessed using an Air-Liquid Interface (ALI) lung infection model based on differentiated NCI-H441 human distal lung epithelial cells cultured on Transwell® inserts. To evaluate the feasibility of aerosol-based delivery, we developed and characterized a liquid formulation of CFS. The aerodynamic performance of nebulized CFS was analyzed using a twin-stage impinger (TSI) and a Next Generation Impactor (NGI), the latter equipped with a breathing simulator to mimic respiratory profiles of both healthy individuals and cystic fibrosis patients. Additionally, the physicochemical and biological stability of CFS was assessed under various storage conditions.

RESULTS

CFS demonstrated significant antibacterial activity in the ALI model, reducing colony-forming units by up to 3 log units after 7 h of incubation, without inducing cytotoxic effects. Scanning electron microscopy confirmed these findings. Aerodynamic testing with the TSI and an Aerogen® mesh nebulizer showed that 76% of the nebulized product was deposited in the second stage, indicating effective deep lung delivery. NGI analysis revealed a favorable aerodynamic particle size distribution (APSD), with a fine particle fraction (FPF) exceeding 60% and a mass median aerodynamic diameter (MMAD) suitable for deep airway deposition. Physicochemical stability studies under stressed temperature conditions predicted prolonged physical stability for CFS at 25°C and demonstrated that they retained anti-pseudomonal activity after 1 year of storage at room temperature, 4°C, and -20°C.

CONCLUSION

These findings support the potential of GG-derived CFS as a promising candidate for inhaled therapy against lung infections. Further validation in animal models is warranted to confirm its therapeutic efficacy and safety , potentially contributing to the development of novel localized treatment strategies for respiratory infections.

摘要

目的

鉴于多重耐药病原体的患病率不断上升以及传统抗生素的疗效不断下降,本研究探讨了益生菌或其代谢产物作为替代抗菌剂的潜力。具体而言,我们研究了源自益生菌菌株GG的无细胞上清液(CFS)对肺部感染局部治疗的抗菌特性。

方法

为模拟人体呼吸环境,我们采用了多种模型。基于在Transwell®小室上培养的分化NCI-H441人远端肺上皮细胞,使用气液界面(ALI)肺部感染模型评估CFS的细胞毒性和抗菌活性。为评估基于气雾剂递送的可行性,我们开发并表征了CFS的液体制剂。使用两级撞击器(TSI)和下一代撞击器(NGI)分析雾化CFS的空气动力学性能,后者配备呼吸模拟器以模拟健康个体和囊性纤维化患者的呼吸特征。此外,在各种储存条件下评估CFS的物理化学和生物学稳定性。

结果

CFS在ALI模型中表现出显著的抗菌活性,孵育7小时后菌落形成单位减少多达3个对数单位,且未诱导细胞毒性作用。扫描电子显微镜证实了这些发现。使用TSI和Aerogen®网状雾化器进行的空气动力学测试表明,76%的雾化产物沉积在第二阶段,表明有效深部肺部递送。NGI分析显示出良好的空气动力学粒径分布(APSD),细颗粒分数(FPF)超过60%,质量中值空气动力学直径(MMAD)适合深部气道沉积。在应激温度条件下的物理化学稳定性研究预测CFS在25°C下具有延长的物理稳定性,并表明它们在室温、4°C和-20°C下储存1年后仍保留抗铜绿假单胞菌活性。

结论

这些发现支持源自GG的CFS作为吸入治疗肺部感染的有前景候选物的潜力。有必要在动物模型中进行进一步验证以确认其治疗效果和安全性,这可能有助于开发用于呼吸道感染的新型局部治疗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f652/12361147/7cc34c89c8d2/fmicb-16-1630017-g001.jpg

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