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一种用于在医疗保健中传播鲍曼不动杆菌干燥表面生物膜的自动化接触模型。

An automated contact model for transmission of dry surface biofilms of Acinetobacter baumannii in healthcare.

机构信息

School of Biological Sciences, University of Southampton, Southampton, UK; Bioquell UK Ltd, Andover, UK.

Bioquell UK Ltd, Andover, UK.

出版信息

J Hosp Infect. 2023 Nov;141:175-183. doi: 10.1016/j.jhin.2023.06.015. Epub 2023 Jun 20.

DOI:10.1016/j.jhin.2023.06.015
PMID:37348564
Abstract

BACKGROUND

Dry surface biofilms (DSBs) have been recognized across environmental and equipment surfaces in hospitals and could explain how microbial contamination can survive for an extended period and may play a key role in the transmission of hospital-acquired infections. Despite little being known on how they form and proliferate in clinical settings, DSB models for disinfectant efficacy testing exist.

AIM

In this study we develop a novel biofilm model to represent formation within hospitals, by emulating patient to surface interactions.

METHODS

The model generates a DSB through the transmission of artificial human sweat (AHS) and clinically relevant pathogens using a synthetic thumb capable of emulating human contact. The DNA, glycoconjugates and protein composition of the model biofilm, along with structural features of the micro-colonies was determined using fluorescent stains visualized by epifluorescence microscopy and compared with published clinical data.

RESULTS

Micrographs revealed the heterogeneity of the biofilm across the surface; and reveal protein as the principal component within the matrix, followed by glycoconjugates and DNA. The model repeatably transferred trace amounts of micro-organisms and AHS, every 5 min for up to 120 h on to stainless-steel coupons to generate a biofilm model averaging 1.16 × 10 cfu/cm falling within the reported range for clinical DSB (4.20 × 10 to 1.60 × 10 bacteria/cm).

CONCLUSION

Our in vitro DSB model exhibits many phenotypical characteristics and traits to those reported in situ. The model highlights key features often overlooked and the potential for downstream applications such as antibiofilm claims using more realistic microbial challenges.

摘要

背景

干燥表面生物膜(DSB)已在医院的环境和设备表面得到广泛认可,这可以解释微生物污染是如何在较长时间内存活下来的,并且可能在医院获得性感染的传播中起关键作用。尽管人们对其在临床环境中形成和增殖的方式知之甚少,但已经存在用于消毒剂功效测试的 DSB 模型。

目的

本研究通过模拟患者与表面的相互作用,开发了一种新的生物膜模型来代表医院内的形成过程。

方法

该模型通过使用能够模拟人体接触的合成拇指传输人造人汗(AHS)和临床相关病原体来产生 DSB。使用荧光染色通过落射荧光显微镜观察来确定模型生物膜的 DNA、糖缀合物和蛋白质组成,以及微菌落的结构特征,并与已发表的临床数据进行比较。

结果

显微镜照片显示了生物膜在整个表面上的异质性;并揭示了蛋白质是基质中的主要成分,其次是糖缀合物和 DNA。该模型可重复地在不锈钢优惠券上转移痕量的微生物和 AHS,每 5 分钟转移一次,最多可达 120 小时,以生成平均为 1.16×10cfu/cm 的生物膜模型,落在临床 DSB(4.20×10 至 1.60×10 细菌/cm)的报告范围内。

结论

我们的体外 DSB 模型表现出许多表型特征和与原位报告的特征。该模型突出了通常被忽视的关键特征,以及使用更现实的微生物挑战进行抗生物膜声称等下游应用的潜力。

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