In Silico and In Vivo Evaluation of Bacteriophage φEF24C, a Candidate for Treatment of
            <i>Enterococcus faecalis</i>
            Infections

Uchiyama, Jumpei; Rashel, Mohammad; Takemura, Iyo; Wakiguchi, Hiroshi; Matsuzaki, Shigenobu

doi:10.1128/aem.02371-07

Cited by 67 publications

(72 citation statements)

References 45 publications

(55 reference statements)

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“…ORFs 13 and 11 had the second and third greatest quantities, so they were also considered structural proteins. N-terminal processing of the major structural protein, as seen in the major structural protein of the other tailed phage, has not been observed in ORF14 of phage KHP30 (43,(63)(64)(65), although the first 3 amino acid residues of ORF13 seemed to be removed. In contrast, ORFs 3, 12, 17, and 29 were present in minor amounts.…”

Section: Resultsmentioning

confidence: 98%

Characterization of Helicobacter pylori Bacteriophage KHP30

Uchiyama

Takeuchi

Kato

et al. 2013

Appl Environ Microbiol

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Helicobacter pylori inhabits the stomach mucosa and is a causative agent of stomach ulcer and cancer. In general, bacteriophages (phages) are strongly associated with bacterial evolution, including the development of pathogenicity. Several tailed phages have so far been reported in H. pylori. We have isolated an H. pylori phage, KHP30, and reported its genomic sequence. In this study, we examined the biological characteristics of phage KHP30. Phage KHP30 was found to be a spherical lipid-containing phage with a diameter of ca. 69 nm. Interestingly, it was stable from pH 2.5 to pH 10, suggesting that it is adapted to the highly acidic environment of the human stomach. Phage KHP30 multiplied on 63.6% of clinical H. pylori isolates. The latent period was ca. 140 min, shorter than the doubling time of H. pylori (ca. 180 min). The burst size was ca. 13, which was smaller than the burst sizes of other known tailed or spherical phages. Phage KHP30 seemed to be maintained as an episome in H. pylori strain NY43 cells, despite a predicted integrase gene in the KHP30 genomic sequence. Seven possible virion proteins of phage KHP30 were analyzed using N-terminal protein sequencing and mass spectrometry, and their genes were found to be located on its genomic DNA. The genomic organization of phage KHP30 differed from the genomic organizations in the known spherical phage families Corticoviridae and Tectiviridae. This evidence suggests that phage KHP30 is a new type of spherical phage that cannot be classified in any existing virus category. Helicobacter pylori, a Gram-negative spiral bacterium, colonizes the human stomach mucosa (1). It causes chronic inflammation, which may progress to peptic ulceration, atrophic gastritis, and gastric cancer (2). Recent studies of H. pylori have revealed that the pathogenicity of H. pylori strains is related to the specific geographic region from which they derive (3, 4). An East Asian type of H. pylori strain most likely causes gastric cancer and highly likely contains cytotoxin-associated gene A (cagA), a carcinogenic genetic element (1, 3). However, how the pathogenicity of the H. pylori strains has evolved is unknown, although H. pylori inhabits a very restricted niche in the stomach mucosa. Therefore, the factors involved in H. pylori evolution must be investigated.Bacteriophages (phages) are the most diverse and abundant life form on Earth. Phages practice lateral gene transfer and are involved in a coevolutionary arms race with bacteria (5-8), so they may well be factors involved in bacterial evolution. Several H. pylori phages have been reported (9-13), and some of these have been morphologically studied and have been found to belong to the order Caudovirales (i.e., the tailed phages) (9-12). Recent advances in sequencing technologies have allowed intensive genomic analyses of Helicobacter spp. and have also suggested the presence of phages in the bacterial genome (10,11,14,15). However, the biological characteristics of these H. pylori phages are not well-known.We have recently iso...

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Section: Resultsmentioning

confidence: 98%

Characterization of Helicobacter pylori Bacteriophage KHP30

Uchiyama

Takeuchi

Kato

et al. 2013

Appl Environ Microbiol

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“…Interestingly, the extent of terminal redundancy in these otherwise similar phages varies greatly, from 3.1 kb in A511 to approximately 20 kb in K. In fact, our data indicate that this is a general feature of the SPO1-like phages. The sequence of Enterococcus faecalis phage EF24C has been published very recently (60) and features significant homologies to A511 (47% overall nucleic acid identity and 64 proteins with Ͼ33.7% identity [expectation values of Ͻ0.001]). Although EF24C was classified as being a SPO1-like phage, the authors of that publication assumed that it has a circularly permuted genome.…”

Section: Discussionmentioning

confidence: 99%

The Terminally Redundant, Nonpermuted Genome ofListeriaBacteriophage A511: a Model for the SPO1-Like Myoviruses of Gram-Positive Bacteria

et al. 2008

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Only little information on a particular class of myoviruses, the SPO1-like bacteriophages infecting low-G؉C-content, gram-positive host bacteria (Firmicutes), is available. We present the genome analysis and molecular characterization of the large, virulent, broad-host-range Listeria phage A511. A511 contains a unit (informational) genome of 134,494 bp, encompassing 190 putative open reading frames (ORFs) and 16 tRNA genes, organized in a modular fashion common among the Caudovirales. Electron microscopy, enzymatic fragmentation analyses, and sequencing revealed that the A511 DNA molecule contains linear terminal repeats of a total of 3,125 bp, encompassing nine small putative ORFs. This particular genome structure explains why A511 is unable to perform general transduction. A511 features significant sequence homologies to Listeria phage P100 and other morphologically related phages infecting Firmicutes such as Staphylococcus phage K and Lactobacillus phage LP65. Equivalent but more-extensive terminal repeats also exist in phages P100 (ϳ6 kb) and K (ϳ20 kb). High-resolution electron microscopy revealed, for the first time, the presence of long tail fibers organized in a sixfold symmetry in these viruses. Mass spectrometry-based peptide fingerprinting permitted assignment of individual proteins to A511 structural components. On the basis of the data available for A511 and relatives, we propose that SPO1-like myoviruses are characterized by (i) their infection of gram-positive, low-G؉C-content bacteria; (ii) a wide host range within the host bacterial genus and a strictly virulent lifestyle; (iii) similar morphology, sequence relatedness, and collinearity of the phage genome organization; and (iv) large double-stranded DNA genomes featuring nonpermuted terminal repeats of various sizes.Listeria monocytogenes is a gram-positive, opportunistic pathogen that can cause a wide spectrum of diseases, such as meningitis, septicemia, abortion, and gastroenteritis, associated with mortality rates as high as 25 to 30% (17, 62). Listeria bacteria are ubiquitously found in nature and can enter the food chain at many points (26, 66). They are able to proliferate over a wide range of external conditions, including low temperatures and high salt concentrations, thus posing severe problems to the food industry (2,22,15,48).Almost all of the Listeria bacteriophages described to date are temperate (38); only very little is known about virulent phages infecting this host. Listeria phages are valuable sources of biological information and useful tools for the study, differentiation, manipulation, and control of these bacteria (6,33,41). Phage A511 and some of its components have been particularly useful in phage typing schemes (35, 61), as reporter phage (39), with respect to their endolysins (16), and also for the control of Listeria contamination of foods (7; S. Guenther, D. Huwyler, S. Richard, and M. J. Loessner, submitted for publication). In contrast to temperate Listeria phages A118 and PSA (36, 71), A511 is a virulent (i.e., s...

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“…[49], vancomycin-resistant Enterococci [50][51][52], antibiotic-resistant Staphylococci [53,54], multidrugresistant Klebsiella pneumonia [55], imipenem-resistant [56,57] and multidrug-resistant Pseudomonas aeruginosa [58,59], antibiotic-resistant strains of Escherichia coli [60], and methicillin-resistant Staphylococcus aureus [61]. Today, there are several different antibacterial strategies derived from phages including enzybiotics (cloned host-specific, phageencoded lytic enzymes introduced to combat bacteria without the whole phage) and whole-phage therapy (introducing whole, viable phage to attack the infecting bacteria) [8,[62][63][64].…”

Section: Medical and Therapeutic Application Of Bacteriophagesmentioning

confidence: 99%

Bacteriophages and Their Derivatives as Biotherapeutic Agents in Disease Prevention and Treatment

et al. 2014

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The application of bacteriophages for the elimination of pathogenic bacteria has received significantly increased attention worldwide in the past decade. This is borne out by the increasing prevalence of bacteriophage-specific conferences highlighting significant and diverse advances in the exploitation of bacteriophages. While bacteriophage therapy has been associated with the Former Soviet Union historically, since the 1990s, it has been widely and enthusiastically adopted as a research topic in Western countries. This has been justified by the increasing prevalence of antibiotic resistance in many prominent human pathogenic bacteria. Discussion of the therapeutic aspects of bacteriophages in this review will include the uses of whole phages as antibacterials and will also describe studies on the applications of purified phage-derived peptidoglycan hydrolases, which do not have the constraint of limited bacterial host-range often observed with whole phages.

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In Silico and In Vivo Evaluation of Bacteriophage φEF24C, a Candidate for Treatment of Enterococcus faecalis Infections

Cited by 67 publications

References 45 publications

Characterization of Helicobacter pylori Bacteriophage KHP30

Characterization of Helicobacter pylori Bacteriophage KHP30

The Terminally Redundant, Nonpermuted Genome ofListeriaBacteriophage A511: a Model for the SPO1-Like Myoviruses of Gram-Positive Bacteria

Bacteriophages and Their Derivatives as Biotherapeutic Agents in Disease Prevention and Treatment

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