Research Portal

CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials

Research output: Contribution to journalArticlepeer-review

Standard Standard

CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials. / Townsend, Eleanor M; Moat, John; Jameson, Eleanor.
In: Biofilm, Vol. 2, 100038, 01.12.2020.

Research output: Contribution to journalArticlepeer-review

HarvardHarvard

Townsend, EM, Moat, J & Jameson, E 2020, 'CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials', Biofilm, vol. 2, 100038. https://doi.org/10.1016/j.bioflm.2020.100038

APA

Townsend, E. M., Moat, J., & Jameson, E. (2020). CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials. Biofilm, 2, Article 100038. https://doi.org/10.1016/j.bioflm.2020.100038

CBE

Townsend EM, Moat J, Jameson E. 2020. CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials. Biofilm. 2:Article 100038. https://doi.org/10.1016/j.bioflm.2020.100038

MLA

Townsend, Eleanor M, John Moat, and Eleanor Jameson. "CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials". Biofilm. 2020. 2. https://doi.org/10.1016/j.bioflm.2020.100038

VancouverVancouver

Townsend EM, Moat J, Jameson E. CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials. Biofilm. 2020 Dec 1;2:100038. Epub 2020 Nov 11. doi: 10.1016/j.bioflm.2020.100038

Author

Townsend, Eleanor M ; Moat, John ; Jameson, Eleanor. / CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials. In: Biofilm. 2020 ; Vol. 2.

RIS

TY - JOUR

T1 - CAUTI's next top model - Model dependent Klebsiella biofilm inhibition by bacteriophages and antimicrobials

AU - Townsend, Eleanor M

AU - Moat, John

AU - Jameson, Eleanor

N1 - © 2020 The Author(s).

PY - 2020/12/1

Y1 - 2020/12/1

N2 - Klebsiella infections, including catheter associated urinary tract infections, are a considerable burden on health care systems. This is due to their difficulty to treat, caused by antimicrobial resistance and their ability to form biofilms. In this study, we investigated the use of a Klebsiella phage cocktail to reduce biofilm viability. We used two methodologies to investigate this, a standard 96-well plate assay and a more complicated Foley catheter-based model. The phage cocktail was used alone and in combination with clinically relevant antibiotic treatments. Viability was measured by both a resazurin based stain and colony forming unit counts, of cells sloughed off from the biofilm. We showed that phage infection dynamics and host survival vary significantly in different standard laboratory media, presumably due to the expression of different surface receptors and capsule composition by the bacteria effecting phage binding. This underscores the importance of a realistic model for developing phage therapy. We demonstrate that bacteriophage-based treatments are a viable option for preventing Klebsiella colonisation and biofilm formation on urinary catheters. Phage cocktails were able to significantly reduce the amount of biofilm that formed when they were present during early biofilm formation. The phages used in this study were unable to significantly reduce a pre-formed mature biofilm, despite encoding depolymerases. Phages applied together with antimicrobial treatments, showed synergistic interactions, in some cases the combined treatment was much more effective than antimicrobial treatments alone. We show that phage cocktails have the potential to prevent Klebsiella biofilms in catheters, if used early or as a preventative treatment and will work well alongside standard antibiotics in the treatment of catheter-associated urinary tract infections (CAUTI).

AB - Klebsiella infections, including catheter associated urinary tract infections, are a considerable burden on health care systems. This is due to their difficulty to treat, caused by antimicrobial resistance and their ability to form biofilms. In this study, we investigated the use of a Klebsiella phage cocktail to reduce biofilm viability. We used two methodologies to investigate this, a standard 96-well plate assay and a more complicated Foley catheter-based model. The phage cocktail was used alone and in combination with clinically relevant antibiotic treatments. Viability was measured by both a resazurin based stain and colony forming unit counts, of cells sloughed off from the biofilm. We showed that phage infection dynamics and host survival vary significantly in different standard laboratory media, presumably due to the expression of different surface receptors and capsule composition by the bacteria effecting phage binding. This underscores the importance of a realistic model for developing phage therapy. We demonstrate that bacteriophage-based treatments are a viable option for preventing Klebsiella colonisation and biofilm formation on urinary catheters. Phage cocktails were able to significantly reduce the amount of biofilm that formed when they were present during early biofilm formation. The phages used in this study were unable to significantly reduce a pre-formed mature biofilm, despite encoding depolymerases. Phages applied together with antimicrobial treatments, showed synergistic interactions, in some cases the combined treatment was much more effective than antimicrobial treatments alone. We show that phage cocktails have the potential to prevent Klebsiella biofilms in catheters, if used early or as a preventative treatment and will work well alongside standard antibiotics in the treatment of catheter-associated urinary tract infections (CAUTI).

U2 - 10.1016/j.bioflm.2020.100038

DO - 10.1016/j.bioflm.2020.100038

M3 - Article

C2 - 33381752

VL - 2

JO - Biofilm

JF - Biofilm

SN - 2590-2075

M1 - 100038

ER -