Characterization of biofilm matrix, degradation by DNase treatment and evidence of capsule downregulation in Streptococcus pneumoniae clinical isolates
Characterization of biofilm matrix, degradation by DNase treatment and evidence of capsule downregulation in Streptococcus pneumoniae clinical isolates
Background: Streptococcus pneumoniae is a common respiratory pathogen and a major causative agent of respiratory infections, including otitis media (OM). Pneumococcal biofilms have been demonstrated on biopsies of the middle ear mucosa in children receiving tympanostomy tubes, supporting the hypothesis that chronic OM may involve biofilm development by pathogenic bacteria as part of the infectious process. To better understand pneumococcal biofilm formation six low-passage encapsulated nasopharyngeal isolates of S. pneumoniae were assessed over a six-eight day period in vitro.
Results: multiparametric analysis divided the strains into two groups. Those with a high biofilm forming index (BFI) were structurally complex, exhibited greater lectin colocalization and were more resistant to azithromycin. Those with a low BFI developed less extensive biofilms and were more susceptible to azithromycin. dsDNA was present in the S. pneumoniae biofilm matrix in all strains and treatment with DNase I significantly reduced biofilm biomass. Since capsule expression has been hypothesized to be associated with decreased biofilm development, we also examined expression of cpsA, the first gene in the pneumococcal capsule operon. Interestingly, cpsA was downregulated in biofilms in both high and low BFI strains.
Conclusion: all pneumococcal strains developed biofilms that exhibited extracellular dsDNA in the biofilm matrix, however strains with a high BFI correlated with greater carbohydrate-associated structural complexity and antibiotic resistance. Furthermore, all strains of S. pneumoniae showed downregulation of the cpsA gene during biofilm growth compared to planktonic culture, regardless of BFI ranking, suggesting downregulation of capsule expression occurs generally during adherent growth.
173-189
Hall-Stoodley, Luanne
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Nistico, Laura
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Sambanthamoorthy, Karthik
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Dice, Bethany
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Nguyen, Duc
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Mershon, William J.
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Johnson, Candice
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Hu, Fan Ze
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Stoodley, Paul
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Ehrlich, Garth D.
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Post, J. Christopher
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8 October 2008
Hall-Stoodley, Luanne
94ebdc00-b549-4488-b15f-5310fb965f5b
Nistico, Laura
7a83886a-6bf1-46a1-87dd-75a120d41603
Sambanthamoorthy, Karthik
e78c92eb-9ff8-4fd3-9ab2-2d52f7084d0b
Dice, Bethany
72120cd5-bde7-4799-bba8-38cc906d14b1
Nguyen, Duc
f6972580-bc57-40b5-b634-4213bbd1e32a
Mershon, William J.
669e9633-de54-4582-ae13-3cd1d5687459
Johnson, Candice
97a0c6f3-977e-4a76-a929-f084b44f6af0
Hu, Fan Ze
bc3be06e-52ac-417d-95b6-c8026fabb2e5
Stoodley, Paul
08614665-92a9-4466-806e-20c6daeb483f
Ehrlich, Garth D.
aa8e5162-77a6-4627-a793-acd724ed0782
Post, J. Christopher
832cfa58-9254-4396-8c8f-6fb18cc6c18c
Hall-Stoodley, Luanne, Nistico, Laura, Sambanthamoorthy, Karthik, Dice, Bethany, Nguyen, Duc, Mershon, William J., Johnson, Candice, Hu, Fan Ze, Stoodley, Paul, Ehrlich, Garth D. and Post, J. Christopher
(2008)
Characterization of biofilm matrix, degradation by DNase treatment and evidence of capsule downregulation in Streptococcus pneumoniae clinical isolates.
BMC Microbiology, 8 (8), .
(doi:10.1186/1471-2180-8-173).
Abstract
Background: Streptococcus pneumoniae is a common respiratory pathogen and a major causative agent of respiratory infections, including otitis media (OM). Pneumococcal biofilms have been demonstrated on biopsies of the middle ear mucosa in children receiving tympanostomy tubes, supporting the hypothesis that chronic OM may involve biofilm development by pathogenic bacteria as part of the infectious process. To better understand pneumococcal biofilm formation six low-passage encapsulated nasopharyngeal isolates of S. pneumoniae were assessed over a six-eight day period in vitro.
Results: multiparametric analysis divided the strains into two groups. Those with a high biofilm forming index (BFI) were structurally complex, exhibited greater lectin colocalization and were more resistant to azithromycin. Those with a low BFI developed less extensive biofilms and were more susceptible to azithromycin. dsDNA was present in the S. pneumoniae biofilm matrix in all strains and treatment with DNase I significantly reduced biofilm biomass. Since capsule expression has been hypothesized to be associated with decreased biofilm development, we also examined expression of cpsA, the first gene in the pneumococcal capsule operon. Interestingly, cpsA was downregulated in biofilms in both high and low BFI strains.
Conclusion: all pneumococcal strains developed biofilms that exhibited extracellular dsDNA in the biofilm matrix, however strains with a high BFI correlated with greater carbohydrate-associated structural complexity and antibiotic resistance. Furthermore, all strains of S. pneumoniae showed downregulation of the cpsA gene during biofilm growth compared to planktonic culture, regardless of BFI ranking, suggesting downregulation of capsule expression occurs generally during adherent growth.
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Published date: 8 October 2008
Organisations:
Engineering Mats & Surface Engineerg Gp
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Local EPrints ID: 155229
URI: http://eprints.soton.ac.uk/id/eprint/155229
PURE UUID: 49affea5-07fd-4a9e-b7f0-a1199df8fe9b
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Date deposited: 27 May 2010 10:42
Last modified: 14 Mar 2024 02:55
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Author:
Luanne Hall-Stoodley
Author:
Laura Nistico
Author:
Karthik Sambanthamoorthy
Author:
Bethany Dice
Author:
Duc Nguyen
Author:
William J. Mershon
Author:
Candice Johnson
Author:
Fan Ze Hu
Author:
Garth D. Ehrlich
Author:
J. Christopher Post
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