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"Anders, Kirk R"

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Pope, W. H., Anders, K. R., Baird, M. A., Bowman, C. A., Boyle, M. M., Broussard, G. W., Chow, T. W., Clase, K., Cooper, S. D., Cornely, K., Dejong, R. J., Delesalle, V. A., Deng, L., Dunbar, D., Edgington, N. P., Ferreira, C. M., Hafer, K. W., Hartzog, G. A., Hatherill, J. R., … Hatfull, G. F. (2014). Cluster M mycobacteriophages Bongo, PegLeg, and Rey with unusually large repertoires of tRNA isotypes. Journal of Virology, 88(5), 2461–2480. https://doi.org/10.1128/JVI.03363-13

Genomic analysis of a large set of phages infecting the common host Mycobacterium smegmatis mc2155 shows that they span considerable genetic diversity. There are more than 20 distinct types that lack nucleotide similarity with each other, and there is considerable diversity within most of the groups. Three newly isolated temperate mycobacteriophages, Bongo, PegLeg, and Rey, constitute a new group (cluster M), with the closely related phages Bongo and PegLeg forming subcluster M1 and the more distantly related Rey forming subcluster M2. The clusterMmycobacteriophages have siphoviral morphologies with unusually long tails, are homoimmune, and have larger than average genomes (80.2 to 83.7 kbp). They exhibit a variety of features not previously described in other mycobacteriophages, including noncanonical genome architectures and several unusual sets of conserved repeated sequences suggesting novel regulatory systems for both transcription and translation. In addition to containing transfer-messenger RNA and RtcB-like RNA ligase genes, their genomes encode 21 to 24 tRNA genes encompassing complete or nearly complete sets of isotypes. We predict that these tRNAs are used in late lytic growth, likely compensating for the degradation or inadequacy of host tRNAs. They may represent a complete set of tRNAs necessary for late lytic growth, especially when taken together with the apparent lack of codons in the same late genes that correspond to tRNAs that the genomes of the phages do not obviously encode. © 2014, American Society for Microbiology.

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Jacobs-Sera, D., Abad, L. A., Alvey, R. M., Anders, K. R., Aull, H. G., Bhalla, S. S., Blumer, L. S., Bollivar, D. W., Bonilla, J. A., Butela, K. A., Coomans, R. J., Cresawn, S. G., D’Elia, T., Diaz, A., Divens, A. M., Edgington, N. P., Frederick, G. D., Gainey, M. D., Garlena, R. A., … Hatfull, G. F. (2020). Genomic diversity of bacteriophages infecting Microbacterium spp. PloS One, 15(6), e0234636. https://doi.org/10/ghts3p

The bacteriophage population is vast, dynamic, old, and genetically diverse. The genomics of phages that infect bacterial hosts in the phylum Actinobacteria show them to not only be diverse but also pervasively mosaic, and replete with genes of unknown function. To further explore this broad group of bacteriophages, we describe here the isolation and genomic characterization of 116 phages that infect Microbacterium spp. Most of the phages are lytic, and can be grouped into twelve clusters according to their overall relatedness; seven of the phages are singletons with no close relatives. Genome sizes vary from 17.3 kbp to 97.7 kbp, and their G+C% content ranges from 51.4% to 71.4%, compared to ~67% for their Microbacterium hosts. The phages were isolated on five different Microbacterium species, but typically do not efficiently infect strains beyond the one on which they were isolated. These Microbacterium phages contain many novel features, including very large viral genes (13.5 kbp) and unusual fusions of structural proteins, including a fusion of VIP2 toxin and a MuF-like protein into a single gene. These phages and their genetic components such as integration systems, recombineering tools, and phage-mediated delivery systems, will be useful resources for advancing Microbacterium genetics.

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