Distinct bacterial population dynamics and disease dissemination after biofilm dispersal and disassembly

Yeping Ma; Yanlin Deng; Haojun Hua; Bee Luan Khoo; Song Lin Chua

doi:10.1038/s41396-023-01446-5

Distinct bacterial population dynamics and disease dissemination after biofilm dispersal and disassembly

Yeping Ma, Yanlin Deng, Haojun Hua, Bee Luan Khoo^*, Song Lin Chua^*

^*Corresponding author for this work

Department of Biomedical Engineering

Research output: Journal Publications and Reviews › RGC 21 - Publication in refereed journal › peer-review

15 Citations (Scopus)

Abstract

Microbial communities that form surface-attached biofilms must release and disperse their constituent cells into the environment to colonize fresh sites for continued survival of their species. For pathogens, biofilm dispersal is crucial for microbial transmission from environmental reservoirs to hosts, cross-host transmission, and dissemination of infections across tissues within the host. However, research on biofilm dispersal and its consequences in colonization of fresh sites remain poorly understood. Bacterial cells can depart from biofilms via stimuli-induced dispersal or disassembly due to direct degradation of the biofilm matrix, but the complex heterogeneity of bacterial populations released from biofilms rendered their study difficult. Using a novel 3D-bacterial “biofilm-dispersal-then-recolonization” (BDR) microfluidic model, we demonstrated that Pseudomonas aeruginosa biofilms undergo distinct spatiotemporal dynamics during chemical-induced dispersal (CID) and enzymatic disassembly (EDA), with contrasting consequences in recolonization and disease dissemination. Active CID required bacteria to employ bdlA dispersal gene and flagella to depart from biofilms as single cells at consistent velocities but could not recolonize fresh surfaces. This prevented the disseminated bacteria cells from infecting lung spheroids and Caenorhabditis elegans in on-chip coculture experiments. In contrast, EDA by degradation of a major biofilm exopolysaccharide (Psl) released immotile aggregates at high initial velocities, enabling the bacteria to recolonize fresh surfaces and cause infections in the hosts efficiently. Hence, biofilm dispersal is more complex than previously thought, where bacterial populations adopting distinct behavior after biofilm departure may be the key to survival of bacterial species and dissemination of diseases. © 2023, The Author(s), under exclusive licence to International Society for Microbial Ecology.

Original language	English
Pages (from-to)	1290–1302
Journal	The ISME Journal
Volume	17
Issue number	8
Online published	3 Jun 2023
DOIs	https://doi.org/10.1038/s41396-023-01446-5
Publication status	Published - Aug 2023

Funding

This research is supported by The Hong Kong Polytechnic University, Department of Applied Biology and Chemical Technology Startup Grant (BE2B), Departmental General Research Fund (UALB), One-line account (ZVVV), Environmental and Conservation Fund (ECF-48/2019 and ECF-84/2021), Health and Medical Research Fund (HMRF-20190302), and State Key Laboratory of Chemical Biology and Drug Discovery Fund (1-BBX8). This work was also supported by the City University of Hong Kong [7005208,7005464,7020002,9610430,9667220]; Hong Kong Center for Cerebro- Cardiovascular Health Engineering (COCHE); Research Grants Council of the Hong Kong Special Administrative Region [21200921]; Pneumoconiosis Compensation Fund Board [9211276]; and the Hetao Shenzhen-Hong Kong Science and Technology Innovation Cooperation Zone Shenzhen Park Project (HZQB-KCZYZ-2021017).

Access Output

10.1038/s41396-023-01446-5

Other Access Options

Check CityUHK Library

Permanent Link

Right click to copy link

Cite this

@article{be7dabd45e5140d9b41c5280e039f60c,

title = "Distinct bacterial population dynamics and disease dissemination after biofilm dispersal and disassembly",

abstract = "Microbial communities that form surface-attached biofilms must release and disperse their constituent cells into the environment to colonize fresh sites for continued survival of their species. For pathogens, biofilm dispersal is crucial for microbial transmission from environmental reservoirs to hosts, cross-host transmission, and dissemination of infections across tissues within the host. However, research on biofilm dispersal and its consequences in colonization of fresh sites remain poorly understood. Bacterial cells can depart from biofilms via stimuli-induced dispersal or disassembly due to direct degradation of the biofilm matrix, but the complex heterogeneity of bacterial populations released from biofilms rendered their study difficult. Using a novel 3D-bacterial “biofilm-dispersal-then-recolonization” (BDR) microfluidic model, we demonstrated that Pseudomonas aeruginosa biofilms undergo distinct spatiotemporal dynamics during chemical-induced dispersal (CID) and enzymatic disassembly (EDA), with contrasting consequences in recolonization and disease dissemination. Active CID required bacteria to employ bdlA dispersal gene and flagella to depart from biofilms as single cells at consistent velocities but could not recolonize fresh surfaces. This prevented the disseminated bacteria cells from infecting lung spheroids and Caenorhabditis elegans in on-chip coculture experiments. In contrast, EDA by degradation of a major biofilm exopolysaccharide (Psl) released immotile aggregates at high initial velocities, enabling the bacteria to recolonize fresh surfaces and cause infections in the hosts efficiently. Hence, biofilm dispersal is more complex than previously thought, where bacterial populations adopting distinct behavior after biofilm departure may be the key to survival of bacterial species and dissemination of diseases. {\textcopyright} 2023, The Author(s), under exclusive licence to International Society for Microbial Ecology.",

author = "Yeping Ma and Yanlin Deng and Haojun Hua and Khoo, {Bee Luan} and Chua, {Song Lin}",

year = "2023",

month = aug,

doi = "10.1038/s41396-023-01446-5",

language = "English",

volume = "17",

pages = "1290–1302",

journal = "The ISME Journal",

issn = "1751-7362",

publisher = "Oxford University Press",

number = "8",

}

TY - JOUR

T1 - Distinct bacterial population dynamics and disease dissemination after biofilm dispersal and disassembly

AU - Ma, Yeping

AU - Deng, Yanlin

AU - Hua, Haojun

AU - Khoo, Bee Luan

AU - Chua, Song Lin

PY - 2023/8

Y1 - 2023/8

N2 - Microbial communities that form surface-attached biofilms must release and disperse their constituent cells into the environment to colonize fresh sites for continued survival of their species. For pathogens, biofilm dispersal is crucial for microbial transmission from environmental reservoirs to hosts, cross-host transmission, and dissemination of infections across tissues within the host. However, research on biofilm dispersal and its consequences in colonization of fresh sites remain poorly understood. Bacterial cells can depart from biofilms via stimuli-induced dispersal or disassembly due to direct degradation of the biofilm matrix, but the complex heterogeneity of bacterial populations released from biofilms rendered their study difficult. Using a novel 3D-bacterial “biofilm-dispersal-then-recolonization” (BDR) microfluidic model, we demonstrated that Pseudomonas aeruginosa biofilms undergo distinct spatiotemporal dynamics during chemical-induced dispersal (CID) and enzymatic disassembly (EDA), with contrasting consequences in recolonization and disease dissemination. Active CID required bacteria to employ bdlA dispersal gene and flagella to depart from biofilms as single cells at consistent velocities but could not recolonize fresh surfaces. This prevented the disseminated bacteria cells from infecting lung spheroids and Caenorhabditis elegans in on-chip coculture experiments. In contrast, EDA by degradation of a major biofilm exopolysaccharide (Psl) released immotile aggregates at high initial velocities, enabling the bacteria to recolonize fresh surfaces and cause infections in the hosts efficiently. Hence, biofilm dispersal is more complex than previously thought, where bacterial populations adopting distinct behavior after biofilm departure may be the key to survival of bacterial species and dissemination of diseases. © 2023, The Author(s), under exclusive licence to International Society for Microbial Ecology.

AB - Microbial communities that form surface-attached biofilms must release and disperse their constituent cells into the environment to colonize fresh sites for continued survival of their species. For pathogens, biofilm dispersal is crucial for microbial transmission from environmental reservoirs to hosts, cross-host transmission, and dissemination of infections across tissues within the host. However, research on biofilm dispersal and its consequences in colonization of fresh sites remain poorly understood. Bacterial cells can depart from biofilms via stimuli-induced dispersal or disassembly due to direct degradation of the biofilm matrix, but the complex heterogeneity of bacterial populations released from biofilms rendered their study difficult. Using a novel 3D-bacterial “biofilm-dispersal-then-recolonization” (BDR) microfluidic model, we demonstrated that Pseudomonas aeruginosa biofilms undergo distinct spatiotemporal dynamics during chemical-induced dispersal (CID) and enzymatic disassembly (EDA), with contrasting consequences in recolonization and disease dissemination. Active CID required bacteria to employ bdlA dispersal gene and flagella to depart from biofilms as single cells at consistent velocities but could not recolonize fresh surfaces. This prevented the disseminated bacteria cells from infecting lung spheroids and Caenorhabditis elegans in on-chip coculture experiments. In contrast, EDA by degradation of a major biofilm exopolysaccharide (Psl) released immotile aggregates at high initial velocities, enabling the bacteria to recolonize fresh surfaces and cause infections in the hosts efficiently. Hence, biofilm dispersal is more complex than previously thought, where bacterial populations adopting distinct behavior after biofilm departure may be the key to survival of bacterial species and dissemination of diseases. © 2023, The Author(s), under exclusive licence to International Society for Microbial Ecology.

UR - http://www.scopus.com/inward/record.url?scp=85160824463&partnerID=8YFLogxK

UR - https://www.scopus.com/record/pubmetrics.uri?eid=2-s2.0-85160824463&origin=recordpage

U2 - 10.1038/s41396-023-01446-5

DO - 10.1038/s41396-023-01446-5

M3 - RGC 21 - Publication in refereed journal

C2 - 37270584

SN - 1751-7362

VL - 17

SP - 1290

EP - 1302

JO - The ISME Journal

JF - The ISME Journal

IS - 8

ER -

Distinct bacterial population dynamics and disease dissemination after biofilm dispersal and disassembly

Abstract

Funding

Access Output

Other Access Options

Permanent Link

Other Files and Links

Fingerprint

ECS: Microfluidic Inflammatory Tumor Model for Drug Discovery in Patients with Systemic Infection

HKgovt: Enrichment of Epithelial Mesothelioma Cell Clusters for Early Detection and Routine Monitoring of Patients Using Liquid Biopsy

Cite this

Distinct bacterial population dynamics and disease dissemination after biofilm dispersal and disassembly

Abstract

Funding

Access Output

Other Access Options

Permanent Link

Other Files and Links

Fingerprint

Projects

ECS: Microfluidic Inflammatory Tumor Model for Drug Discovery in Patients with Systemic Infection

HKgovt: Enrichment of Epithelial Mesothelioma Cell Clusters for Early Detection and Routine Monitoring of Patients Using Liquid Biopsy

Cite this