Your search keyword '"Tail fiber"' showing total 9 results

1. Discovery and characterisation of new phage targeting uropathogenic Escherichia coli.

Author

Asgharzadeh Kangachar S, Logel DY, Trofimova E, Zhu HX, Zaugg J, Schembri MA, Weynberg KD, and Jaschke PR

Subjects

Humans, Uropathogenic Escherichia coli genetics, Uropathogenic Escherichia coli virology, Host Specificity, Urinary Tract Infections microbiology, Urinary Tract Infections virology, Escherichia coli Infections microbiology, Escherichia coli Infections virology, Genome, Viral, Phage Therapy, Bacteriophages genetics, Bacteriophages physiology

Abstract

Antimicrobial resistance is an escalating threat with few new therapeutic options in the pipeline. Urinary tract infections (UTIs) are one of the most prevalent bacterial infections globally and are prone to becoming recurrent and antibiotic resistant. We discovered and characterized six novel Autographiviridae and Guernseyvirinae bacterial viruses (phage) against uropathogenic Escherichia coli (UPEC), a leading cause of UTIs. The phage genomes were between 39,471 bp - 45,233 bp, with 45.0%-51.0% GC%, and 57-84 predicted coding sequences per genome. We show that tail fiber domain structure, predicted host capsule type, and host antiphage repertoire correlate with phage host range. In vitro characterisation of phage cocktails showed synergistic improvement against a mixed UPEC strain population and when sequentially dosed. Together, these phage are a new set extending available treatments for UTI from UPEC, and phage vM_EcoM_SHAK9454 represents a promising candidate for further improvement through engineering., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

2. Engineering Phage Host-Range and Suppressing Bacterial Resistance through Phage Tail Fiber Mutagenesis.

Author

Yehl K, Lemire S, Yang AC, Ando H, Mimee M, Torres MT, de la Fuente-Nunez C, and Lu TK

Subjects

Animals, Drug Resistance, Bacterial, Host Specificity, Mice, Mutagenesis, Site-Directed, Bacteriophage T3 genetics, Escherichia coli virology, Escherichia coli Infections therapy, Phage Therapy methods, Skin Diseases, Bacterial therapy, Viral Tail Proteins genetics

Abstract

The rapid emergence of antibiotic-resistant infections is prompting increased interest in phage-based antimicrobials. However, acquisition of resistance by bacteria is a major issue in the successful development of phage therapies. Through natural evolution and structural modeling, we identified host-range-determining regions (HRDRs) in the T3 phage tail fiber protein and developed a high-throughput strategy to genetically engineer these regions through site-directed mutagenesis. Inspired by antibody specificity engineering, this approach generates deep functional diversity while minimizing disruptions to the overall tail fiber structure, resulting in synthetic "phagebodies." We showed that mutating HRDRs yields phagebodies with altered host-ranges, and select phagebodies enable long-term suppression of bacterial growth in vitro, by preventing resistance appearance, and are functional in vivo using a murine model. We anticipate that this approach may facilitate the creation of next-generation antimicrobials that slow resistance development and could be extended to other viral scaffolds for a broad range of applications., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

3. Predictable Molecular Adaptation of Coevolving Enterococcus faecium and Lytic Phage EfV12-phi1

Author

Wandro, Stephen, Oliver, Andrew, Gallagher, Tara, Weihe, Claudia, England, Whitney, Martiny, Jennifer BH, and Whiteson, Katrine

Subjects

Microbiology, Medical Microbiology, Biomedical and Clinical Sciences, Biological Sciences, Genetics, Antimicrobial Resistance, Human Genome, Infectious Diseases, Biotechnology, Aetiology, 2.1 Biological and endogenous factors, Infection, phage, Enterococcus, experimental evolution, phage therapy, tail fiber, exopolysaccharide, coevolution, Environmental Science and Management, Soil Sciences, Medical microbiology

Abstract

Bacteriophages are highly abundant in human microbiota where they coevolve with resident bacteria. Phage predation can drive the evolution of bacterial resistance, which can then drive reciprocal evolution in the phage to overcome that resistance. Such coevolutionary dynamics have not been extensively studied in human gut bacteria, and are of particular interest for both understanding and eventually manipulating the human gut microbiome. We performed experimental evolution of an Enterococcus faecium isolate from healthy human stool in the absence and presence of a single infecting Myoviridae bacteriophage, EfV12-phi1. Four replicates of E. faecium and phage were grown with twice daily serial transfers for 8 days. Genome sequencing revealed that E. faecium evolved resistance to phage through mutations in the yqwD2 gene involved in exopolysaccharide biogenesis and export, and the rpoC gene which encodes the RNA polymerase β' subunit. In response to bacterial resistance, phage EfV12-phi1 evolved varying numbers of 1.8 kb tandem duplications within a putative tail fiber gene. Host range assays indicated that coevolution of this phage-host pair resulted in arms race dynamics in which bacterial resistance and phage infectivity increased over time. Tracking mutations from population sequencing of experimental coevolution can quickly illuminate phage entry points along with resistance strategies in both phage and host - critical information for using phage to manipulate microbial communities.

Published

2019

4. Predictable Molecular Adaptation of Coevolving Enterococcus faecium and Lytic Phage EfV12-phi1.

Author

Wandro, Stephen, Oliver, Andrew, Gallagher, Tara, Weihe, Claudia, England, Whitney, Martiny, Jennifer BH, and Whiteson, Katrine

Subjects

Enterococcus, coevolution, exopolysaccharide, experimental evolution, phage, phage therapy, tail fiber, Environmental Science and Management, Soil Sciences, Microbiology

Abstract

Bacteriophages are highly abundant in human microbiota where they coevolve with resident bacteria. Phage predation can drive the evolution of bacterial resistance, which can then drive reciprocal evolution in the phage to overcome that resistance. Such coevolutionary dynamics have not been extensively studied in human gut bacteria, and are of particular interest for both understanding and eventually manipulating the human gut microbiome. We performed experimental evolution of an Enterococcus faecium isolate from healthy human stool in the absence and presence of a single infecting Myoviridae bacteriophage, EfV12-phi1. Four replicates of E. faecium and phage were grown with twice daily serial transfers for 8 days. Genome sequencing revealed that E. faecium evolved resistance to phage through mutations in the yqwD2 gene involved in exopolysaccharide biogenesis and export, and the rpoC gene which encodes the RNA polymerase β' subunit. In response to bacterial resistance, phage EfV12-phi1 evolved varying numbers of 1.8 kb tandem duplications within a putative tail fiber gene. Host range assays indicated that coevolution of this phage-host pair resulted in arms race dynamics in which bacterial resistance and phage infectivity increased over time. Tracking mutations from population sequencing of experimental coevolution can quickly illuminate phage entry points along with resistance strategies in both phage and host - critical information for using phage to manipulate microbial communities.

Published

2018

5. Predictable Molecular Adaptation of Coevolving Enterococcus faecium and Lytic Phage EfV12-phi1

Author

Stephen Wandro, Andrew Oliver, Tara Gallagher, Claudia Weihe, Whitney England, Jennifer B. H. Martiny, and Katrine Whiteson

Subjects

phage (bacteriophage), Enterococcus, experimental evolution, phage therapy, tail fiber, exopolysaccharide, Microbiology, QR1-502

Abstract

Bacteriophages are highly abundant in human microbiota where they coevolve with resident bacteria. Phage predation can drive the evolution of bacterial resistance, which can then drive reciprocal evolution in the phage to overcome that resistance. Such coevolutionary dynamics have not been extensively studied in human gut bacteria, and are of particular interest for both understanding and eventually manipulating the human gut microbiome. We performed experimental evolution of an Enterococcus faecium isolate from healthy human stool in the absence and presence of a single infecting Myoviridae bacteriophage, EfV12-phi1. Four replicates of E. faecium and phage were grown with twice daily serial transfers for 8 days. Genome sequencing revealed that E. faecium evolved resistance to phage through mutations in the yqwD2 gene involved in exopolysaccharide biogenesis and export, and the rpoC gene which encodes the RNA polymerase β’ subunit. In response to bacterial resistance, phage EfV12-phi1 evolved varying numbers of 1.8 kb tandem duplications within a putative tail fiber gene. Host range assays indicated that coevolution of this phage-host pair resulted in arms race dynamics in which bacterial resistance and phage infectivity increased over time. Tracking mutations from population sequencing of experimental coevolution can quickly illuminate phage entry points along with resistance strategies in both phage and host – critical information for using phage to manipulate microbial communities.

Published

2019

6. Genomic analysis and relatedness of P2-like phages of the Burkholderia cepacia complex.

Author

Lynch, Karlene H, Stothard, Paul, and Dennis, Jonathan J

Subjects

*BURKHOLDERIA cepacia, *ENDONUCLEASES, *BACTERIOPHAGES, *REVERSE transcriptase, *LYTIC cycle, *BASE pairs, *BURKHOLDERIA cenocepacia

Abstract

Background: The Burkholderia cepacia complex (BCC) is comprised of at least seventeen Gram-negative species that cause infections in cystic fibrosis patients. Because BCC bacteria are broadly antibiotic resistant, phage therapy is currently being investigated as a possible alternative treatment for these infections. The purpose of our study was to sequence and characterize three novel BCC-specific phages: KS5 (vB_BceM-KS5 or vB_BmuZ-ATCC 17616), KS14 (vB_BceM-KS14) and KL3 (vB_BamM-KL3 or vB_BceZ-CEP511). Results: KS5, KS14 and KL3 are myoviruses with the A1 morphotype. The genomes of these phages are between 32317 and 40555 base pairs in length and are predicted to encode between 44 and 52 proteins. These phages have over 50% of their proteins in common with enterobacteria phage P2 and so can be classified as members of the Peduovirinae subfamily and the "P2-like viruses" genus. The BCC phage proteins similar to those encoded by P2 are predominantly structural components involved in virion morphogenesis. As prophages, KS5 and KL3 integrate into an AMP nucleosidase gene and a threonine tRNA gene, respectively. Unlike other P2-like viruses, the KS14 prophage is maintained as a plasmid. The P2 E+E' translational frameshift site is conserved among these three phages and so they are predicted to use frameshifting for expression of two of their tail proteins. The lysBC genes of KS14 and KL3 are similar to those of P2, but in KS5 the organization of these genes suggests that they may have been acquired via horizontal transfer from a phage similar to λ. KS5 contains two sequence elements that are unique among these three phages: an ISBmu 2-like insertion sequence and a reverse transcriptase gene. KL3 encodes an EcoRII-C endonuclease/methylase pair and Vsr endonuclease that are predicted to function during the lytic cycle to cleave non-self DNA, protect the phage genome and repair methylation-induced mutations. Conclusions: KS5, KS14 and KL3 are the first BCC-specific phages to be identified as P2-like. As KS14 has previously been shown to be active against Burkholderia cenocepacia in vivo, genomic characterization of these phages is a crucial first step in the development of these and similar phages for clinical use against the BCC. [ABSTRACT FROM AUTHOR]

Published

2010

7. Alteromonas Myovirus V22 Represents a New Genus of Marine Bacteriophages Requiring a Tail Fiber Chaperone for Host Recognition

Author

Martin J. Loessner, Ana-Belen Martin-Cuadrado, Juan J. Roda-Garcia, Rafael Gonzalez-Serrano, Francisco Rodriguez-Valera, Virginie Grosboillot, Léa V. Zinsli, Riccardo Rosselli, Matthew Dunne, Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, and Ecología Microbiana Molecular

Subjects

Phage therapy, Physiology, medicine.medical_treatment, viruses, lcsh:QR1-502, Myoviridae, Computational biology, Ecological and Evolutionary Science, Microbiología, Biochemistry, Genome, Microbiology, lcsh:Microbiology, Bacteriophage, Tail fiber chaperone, 03 medical and health sciences, Myoalterovirus, Genetics, medicine, Alteromonas, Phage V22, Host recognition, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Synteny, 0303 health sciences, Receptor binding protein, biology, 030306 microbiology, Host recognitio, Tail fiber, biology.organism_classification, QR1-502, Computer Science Applications, Modeling and Simulation, Chaperone (protein), Viral evolution, biology.protein, host recognition, Research Article

Abstract

Marine phages play a variety of critical roles in regulating the microbial composition of our oceans. Despite constituting the majority of genetic diversity within these environments, there are relatively few isolates with complete genome sequences or in-depth analyses of their host interaction mechanisms, such as characterization of their receptor binding proteins (RBPs). Here, we present the 92,760-bp genome of the Alteromonas-targeting phage V22. Genomic and morphological analyses identify V22 as a myovirus; however, due to a lack of sequence similarity to any other known myoviruses, we propose that V22 be classified as the type phage of a new Myoalterovirus genus within the Myoviridae family. V22 shows gene homology and synteny with two different subfamilies of phages infecting enterobacteria, specifically within the structural region of its genome. To improve our understanding of the V22 adsorption process, we identified putative RBPs (gp23, gp24, and gp26) and tested their ability to decorate the V22 propagation strain, Alteromonas mediterranea PT11, as recombinant green fluorescent protein (GFP)-tagged constructs. Only GFP-gp26 was capable of bacterial recognition and identified as the V22 RBP. Interestingly, production of functional GFP-gp26 required coexpression with the downstream protein gp27. GFP-gp26 could be expressed alone but was incapable of host recognition. By combining size-exclusion chromatography with fluorescence microscopy, we reveal how gp27 is not a component of the final RBP complex but instead is identified as a new type of phage-encoded intermolecular chaperone that is essential for maturation of the gp26 RBP., mSystems, 5 (3), ISSN:2379-5077

Published

2020

8. Characterization and Genomic Analysis of SFPH2, a Novel T7virus Infecting Shigella

Author

Hongbo Liu, Hui Ma, Beibei Liang, Renlong Bao, Lang Yang, Hongbin Song, Leili Jia, Jing Xie, Nian Dong, Shaofu Qiu, Ying Xiang, Chaojie Yang, and Haiying Wang

Subjects

0301 basic medicine, Microbiology (medical), Serotype, Shigellosis, Phage therapy, medicine.medical_treatment, lcsh:QR1-502, medicine.disease_cause, Microbiology, Genome, lcsh:Microbiology, Shigella flexneri, Bacteriophage, 03 medical and health sciences, bacteriophage, medicine, Shigella, genome analysis, biology, biology.organism_classification, medicine.disease, 030104 developmental biology, tail fiber, Lytic cycle, T7virus

Abstract

Shigellosis, caused by Shigella, is a major global health concern, with nearly 164.7 million cases and over a million deaths occurring annually worldwide. Shigella flexneri is one of the most common subgroups of Shigella with a high incidence of multidrug-resistance. The phage therapy approach is an effective method for controlling multidrug-resistant bacteria. However, only a few Shigella phages have been described to date. In this study, a novel lytic bacteriophage SFPH2 was isolated from a sewage sample obtained from a hospital in Beijing, China, using a multidrug-resistant Shigella flexneri 2a strain (SF2) isolated from the fecal sample of a dysentery patient. SFPH2 is a member of the Podoviridae virus family with an icosahedral capsid and a short, non-contractile tail. It was found to be stable over a wide range of temperatures (4 – 50°C) and pH values (pH 3 – 11). Moreover, SFPH2 could infect two other S. flexneri serotypes (serotypes 2 variant and Y). High-throughput sequencing revealed that SFPH2 has a linear double-stranded DNA genome of 40,387 bp with 50 open reading frames. No tRNA genes were identified in the genome. Comparative analysis of the genome revealed that the SFPH2 belongs to the subfamily Autographivirinae and genus T7virus. The genome shows high similarity with other enterobacterial T7virus bacteriophages such as Citrobacter phage SH4 (95% identity and 89% coverage) and Cronobacter phage Dev2 (94% identity and 92% coverage). A comparison of the fiber proteins showed that minor differences in the amino acid residues might specify different protein binding regions and determine host species. In conclusion, this is the first report of a T7virus that can infect Shigella; SFPH2 has a functional stability under a wide range of temperatures and pH values, showing the potential to be widely applied to control Shigella–associated clinical infections and reduce the transmission rates of S. flexneri serotype 2a and its variants in the environment.

Published

2018

9. Molecular modification of T4 bacteriophage proteins and its potential application — Review

Author

Kurzępa, A., Dąbrowska, K., Świtała-Jeleń, K., and Górski, A.

Published

2009