A new model of endotracheal tube biofilm identifies combinations of matrix-degrading enzymes and antimicrobials able to eradicate biofilms of pathogens that cause ventilator-associated pneumonia.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-08-01 DOI:10.1099/mic.0.001480

Dean Walsh, Chris Parmenter, Saskia E Bakker, Trevor Lithgow, Ana Traven, Freya Harrison

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Abstract

Ventilator-associated pneumonia is defined as pneumonia that develops in a patient who has been on mechanical ventilation for more than 48 hours through an endotracheal tube. It is caused by biofilm formation on the indwelling tube, which introduces pathogenic microbes such as Pseudomonas aeruginosa, Klebsiella pneumoniae and Candida albicans into the patient's lower airways. Currently, there is a lack of accurate in vitro models of ventilator-associated pneumonia development. This greatly limits our understanding of how the in-host environment alters pathogen physiology and the efficacy of ventilator-associated pneumonia prevention or treatment strategies. Here, we showcase a reproducible model that simulates the biofilm formation of these pathogens in a host-mimicking environment and demonstrate that the biofilm matrix produced differs from that observed in standard laboratory growth medium. In our model, pathogens are grown on endotracheal tube segments in the presence of a novel synthetic ventilated airway mucus medium that simulates the in-host environment. Matrix-degrading enzymes and cryo-scanning electron microscopy were employed to characterize the system in terms of biofilm matrix composition and structure, as compared to standard laboratory growth medium. As seen in patients, the biofilms of ventilator-associated pneumonia pathogens in our model either required very high concentrations of antimicrobials for eradication or could not be eradicated. However, combining matrix-degrading enzymes with antimicrobials greatly improved the biofilm eradication of all pathogens. Our in vitro endotracheal tube model informs on fundamental microbiology in the ventilator-associated pneumonia context and has broad applicability as a screening platform for antibiofilm measures including the use of matrix-degrading enzymes as antimicrobial adjuvants.

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气管导管生物膜的新模型确定了基质降解酶和抗菌剂的组合，它们能够根除导致呼吸机相关肺炎的病原体生物膜。

呼吸机相关肺炎是指通过气管插管进行机械通气超过 48 小时的患者发生的肺炎。它是由留置管上形成的生物膜将铜绿假单胞菌、肺炎克雷伯氏菌和白色念珠菌等病原微生物带入患者下呼吸道引起的。目前，还缺乏准确的呼吸机相关肺炎体外模型。这极大地限制了我们对宿主环境如何改变病原体生理学以及呼吸机相关肺炎预防或治疗策略疗效的了解。在这里，我们展示了一个可重复的模型，该模型模拟了这些病原体在模拟宿主的环境中形成生物膜的过程，并证明了所形成的生物膜基质与在标准实验室生长培养基中观察到的不同。在我们的模型中，病原体在模拟宿主环境的新型合成通气道粘液培养基存在下生长在气管导管节段上。通过基质降解酶和低温扫描电子显微镜观察生物膜基质的组成和结构，并与标准实验室生长培养基进行比较。正如在病人身上看到的那样，我们的模型中呼吸机相关肺炎病原体的生物膜要么需要高浓度的抗菌素才能根除，要么无法根除。然而，将基质降解酶与抗菌剂结合使用，可大大改善所有病原体的生物膜根除效果。我们的体外气管导管模型为呼吸机相关性肺炎的基本微生物学提供了信息，并可作为抗生物膜措施（包括使用基质降解酶作为抗菌剂佐剂）的筛选平台，具有广泛的适用性。

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