Genomic characterization of four novel bacteriophages infecting the clinical pathogen Klebsiella pneumoniae
Genomic characterization of four novel bacteriophages infecting the clinical pathogen Klebsiella pneumoniae
Bacteriophages are an invaluable source of novel genetic diversity. Sequencing of phage genomes can reveal new proteins with potential uses as biotechnological and medical tools, and help unravel the diversity of biological mechanisms employed by phages to take over the host during viral infection. Aiming to expand the available collection of phage genomes, we have isolated, sequenced, and assembled the genome sequences of four phages that infect the clinical pathogen Klebsiella pneumoniae: vB_KpnP_FBKp16, vB_KpnP_FBKp27, vB_KpnM_FBKp34, and Jumbo phage vB_KpnM_FBKp24. The four phages show very low (0–13%) identity to genomic phage sequences deposited in the GenBank database. Three of the four phages encode tRNAs and have a GC content very dissimilar to that of the host. Importantly, the genome sequences of the phages reveal potentially novel DNA packaging mechanisms as well as distinct clades of tubulin spindle and nucleus shell proteins that some phages use to compartmentalize viral replication. Overall, this study contributes to uncovering previously unknown virus diversity, and provides novel candidates for phage therapy applications against antibiotic-resistant K. pneumoniae infections.
Bonilla, Boris Estrada
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Costa, Ana Rita
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van Rossum, Teunke
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Hagedoom, Stefan
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Walinga, Hielke
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Xiao, Minfeng
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Song, Wenchen
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Haas, Pieter-Jan
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Luzia De Nobrega, Franklin
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Brouns, Stan JJ
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13 August 2021
Bonilla, Boris Estrada
b36a1268-8814-4c20-8212-c66e7ddea57e
Costa, Ana Rita
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van Rossum, Teunke
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Hagedoom, Stefan
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Walinga, Hielke
14669684-93c1-4f29-86fa-0d17fce50822
Xiao, Minfeng
1ddea84b-6e99-48fc-8ec1-7928d5830101
Song, Wenchen
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Haas, Pieter-Jan
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Luzia De Nobrega, Franklin
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Brouns, Stan JJ
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Bonilla, Boris Estrada, Costa, Ana Rita, van Rossum, Teunke, Hagedoom, Stefan, Walinga, Hielke, Xiao, Minfeng, Song, Wenchen, Haas, Pieter-Jan, Luzia De Nobrega, Franklin and Brouns, Stan JJ
(2021)
Genomic characterization of four novel bacteriophages infecting the clinical pathogen Klebsiella pneumoniae.
DNA Research, 28, [dsab013].
(doi:10.1093/dnares/dsab013).
Abstract
Bacteriophages are an invaluable source of novel genetic diversity. Sequencing of phage genomes can reveal new proteins with potential uses as biotechnological and medical tools, and help unravel the diversity of biological mechanisms employed by phages to take over the host during viral infection. Aiming to expand the available collection of phage genomes, we have isolated, sequenced, and assembled the genome sequences of four phages that infect the clinical pathogen Klebsiella pneumoniae: vB_KpnP_FBKp16, vB_KpnP_FBKp27, vB_KpnM_FBKp34, and Jumbo phage vB_KpnM_FBKp24. The four phages show very low (0–13%) identity to genomic phage sequences deposited in the GenBank database. Three of the four phages encode tRNAs and have a GC content very dissimilar to that of the host. Importantly, the genome sequences of the phages reveal potentially novel DNA packaging mechanisms as well as distinct clades of tubulin spindle and nucleus shell proteins that some phages use to compartmentalize viral replication. Overall, this study contributes to uncovering previously unknown virus diversity, and provides novel candidates for phage therapy applications against antibiotic-resistant K. pneumoniae infections.
Text
dsab013
- Version of Record
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Accepted/In Press date: 12 August 2021
Published date: 13 August 2021
Identifiers
Local EPrints ID: 456196
URI: http://eprints.soton.ac.uk/id/eprint/456196
PURE UUID: 68849c8c-cc3e-419e-9274-9e67b081d82a
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Date deposited: 26 Apr 2022 16:46
Last modified: 17 Mar 2024 04:02
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Author:
Boris Estrada Bonilla
Author:
Ana Rita Costa
Author:
Teunke van Rossum
Author:
Stefan Hagedoom
Author:
Hielke Walinga
Author:
Minfeng Xiao
Author:
Wenchen Song
Author:
Pieter-Jan Haas
Author:
Stan JJ Brouns
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