Viable bacterial communities on hospital window components in patient rooms

Previous studies demonstrate an exchange of bacteria between hospital room surfaces and patients, and a reduction in survival of microorganisms in dust inside buildings from sunlight exposure. While the transmission of microorganisms between humans and their local environment is a continuous exchang...

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Main Authors: Patrick F. Horve, Leslie G. Dietz, Suzanne L. Ishaq, Jeff Kline, Mark Fretz, Kevin G. Van Den Wymelenberg
Format: Article
Language:English
Published: PeerJ Inc. 2020-07-01
Series:PeerJ
Subjects:
Online Access:https://peerj.com/articles/9580.pdf
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spelling doaj-570cfcf46a6a4ca194f9aa35fab932b42020-11-25T01:28:31ZengPeerJ Inc.PeerJ2167-83592020-07-018e958010.7717/peerj.9580Viable bacterial communities on hospital window components in patient roomsPatrick F. Horve0Leslie G. Dietz1Suzanne L. Ishaq2Jeff Kline3Mark Fretz4Kevin G. Van Den Wymelenberg5Biology and the Built Environment Center, University of Oregon, Eugene, OR, United States of AmericaBiology and the Built Environment Center, University of Oregon, Eugene, OR, United States of AmericaBiology and the Built Environment Center, University of Oregon, Eugene, OR, United States of AmericaBiology and the Built Environment Center, University of Oregon, Eugene, OR, United States of AmericaInstitute for Health in the Built Environment, University of Oregon, Portland, OR, United States of AmericaBiology and the Built Environment Center, University of Oregon, Eugene, OR, United States of AmericaPrevious studies demonstrate an exchange of bacteria between hospital room surfaces and patients, and a reduction in survival of microorganisms in dust inside buildings from sunlight exposure. While the transmission of microorganisms between humans and their local environment is a continuous exchange which generally does not raise cause for alarm, in a hospital setting with immunocompromised patients, these building-source microbial reservoirs may pose a risk. Window glass is often neglected during hospital disinfection protocols, and the microbial communities found there have not previously been examined. This pilot study examined whether living bacterial communities, and specifically the pathogens Methicillin-resistant Staphylococcus aureus (MRSA) and Clostridioides difficile (C. difficile), were present on window components of exterior-facing windows inside patient rooms, and whether relative light exposure (direct or indirect) was associated with changes in bacterial communities on those hospital surfaces. Environmental samples were collected from 30 patient rooms in a single ward at Oregon Health & Science University (OHSU) in Portland, Oregon, USA. Sampling locations within each room included the window glass surface, both sides of the window curtain, two surfaces of the window frame, and the air return grille. Viable bacterial abundances were quantified using qPCR, and community composition was assessed using Illumina MiSeq sequencing of the 16S rRNA gene V3/V4 region. Viable bacteria occupied all sampled locations, but was not associated with a specific hospital surface or relative sunlight exposure. Bacterial communities were similar between window glass and the rest of the room, but had significantly lower Shannon Diversity, theorized to be related to low nutrient density and resistance to bacterial attachment of glass compared to other surface materials. Rooms with windows that were facing west demonstrated a higher abundance of viable bacteria than those facing other directions, potentially because at the time of sampling (morning) west-facing rooms had not yet been exposed to sunlight that day. Viable C. difficile was not detected and viable MRSA was detected at very low abundance. Bacterial abundance was negatively correlated with distance from the central staff area containing the break room and nursing station. In the present study, it can be assumed that there is more human traffic in the center of the ward, and is likely responsible for the observed gradient of total abundance in rooms along the ward, as healthcare staff both deposit more bacteria during activities and affect microbial transit indoors. Overall, hospital window components possess similar microbial communities to other previously identified room locations known to act as reservoirs for microbial agents of hospital-associated infections.https://peerj.com/articles/9580.pdf16S rRNA geneEnvironmental microbiologyHospital-associated infectionsHospital microbiomeIndoor microbial community
collection DOAJ
language English
format Article
sources DOAJ
author Patrick F. Horve
Leslie G. Dietz
Suzanne L. Ishaq
Jeff Kline
Mark Fretz
Kevin G. Van Den Wymelenberg
spellingShingle Patrick F. Horve
Leslie G. Dietz
Suzanne L. Ishaq
Jeff Kline
Mark Fretz
Kevin G. Van Den Wymelenberg
Viable bacterial communities on hospital window components in patient rooms
PeerJ
16S rRNA gene
Environmental microbiology
Hospital-associated infections
Hospital microbiome
Indoor microbial community
author_facet Patrick F. Horve
Leslie G. Dietz
Suzanne L. Ishaq
Jeff Kline
Mark Fretz
Kevin G. Van Den Wymelenberg
author_sort Patrick F. Horve
title Viable bacterial communities on hospital window components in patient rooms
title_short Viable bacterial communities on hospital window components in patient rooms
title_full Viable bacterial communities on hospital window components in patient rooms
title_fullStr Viable bacterial communities on hospital window components in patient rooms
title_full_unstemmed Viable bacterial communities on hospital window components in patient rooms
title_sort viable bacterial communities on hospital window components in patient rooms
publisher PeerJ Inc.
series PeerJ
issn 2167-8359
publishDate 2020-07-01
description Previous studies demonstrate an exchange of bacteria between hospital room surfaces and patients, and a reduction in survival of microorganisms in dust inside buildings from sunlight exposure. While the transmission of microorganisms between humans and their local environment is a continuous exchange which generally does not raise cause for alarm, in a hospital setting with immunocompromised patients, these building-source microbial reservoirs may pose a risk. Window glass is often neglected during hospital disinfection protocols, and the microbial communities found there have not previously been examined. This pilot study examined whether living bacterial communities, and specifically the pathogens Methicillin-resistant Staphylococcus aureus (MRSA) and Clostridioides difficile (C. difficile), were present on window components of exterior-facing windows inside patient rooms, and whether relative light exposure (direct or indirect) was associated with changes in bacterial communities on those hospital surfaces. Environmental samples were collected from 30 patient rooms in a single ward at Oregon Health & Science University (OHSU) in Portland, Oregon, USA. Sampling locations within each room included the window glass surface, both sides of the window curtain, two surfaces of the window frame, and the air return grille. Viable bacterial abundances were quantified using qPCR, and community composition was assessed using Illumina MiSeq sequencing of the 16S rRNA gene V3/V4 region. Viable bacteria occupied all sampled locations, but was not associated with a specific hospital surface or relative sunlight exposure. Bacterial communities were similar between window glass and the rest of the room, but had significantly lower Shannon Diversity, theorized to be related to low nutrient density and resistance to bacterial attachment of glass compared to other surface materials. Rooms with windows that were facing west demonstrated a higher abundance of viable bacteria than those facing other directions, potentially because at the time of sampling (morning) west-facing rooms had not yet been exposed to sunlight that day. Viable C. difficile was not detected and viable MRSA was detected at very low abundance. Bacterial abundance was negatively correlated with distance from the central staff area containing the break room and nursing station. In the present study, it can be assumed that there is more human traffic in the center of the ward, and is likely responsible for the observed gradient of total abundance in rooms along the ward, as healthcare staff both deposit more bacteria during activities and affect microbial transit indoors. Overall, hospital window components possess similar microbial communities to other previously identified room locations known to act as reservoirs for microbial agents of hospital-associated infections.
topic 16S rRNA gene
Environmental microbiology
Hospital-associated infections
Hospital microbiome
Indoor microbial community
url https://peerj.com/articles/9580.pdf
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