Cluster k mycobacteriophages: Insights into the evolutionary origins of mycobacteriophage tm4

Welkin H. Pope; Christina M. Ferreira; Deborah Jacobs-Sera; Robert C. Benjamin; Ariangela J. Davis; Randall J. DeJong; Sarah C.R. Elgin; Forrest R. Guilfoile; Mark H. Forsyth; Alexander D. Harris; Samuel E. Harvey; Lee E. Hughes; Peter M. Hynes; Arrykka S. Jackson; Marilyn D. Jalal; Elizabeth A. MacMurray; Coreen M. Manley; Molly J. McDonough; Jordan L. Mosier; Larissa J. Osterbann; Hannah S. Rabinowitz; Corwin N. Rhyan; Daniel A. Russell; Margaret S. Saha; Christopher D. Shaffer; Stephanie E. Simon; Erika F. Sims; Isabel G. Tovar; Emilie G. Weisser; John T. Wertz; Kathleen A. Weston-Hafer; Kurt E. Williamson; Bo Zhang; Steven G. Cresawn; Paras Jain; Mariana Piuri; William R. Jacobs; Roger W. Hendrix; Graham F. Hatfull

Journal ArticleOPEN ACCESS

Cluster k mycobacteriophages: Insights into the evolutionary origins of mycobacteriophage tm4

PLoS ONE (2011) 6(10)

DOI: 10.1371/journal.pone.0026750

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Abstract

Five newly isolated mycobacteriophages -Angelica, CrimD, Adephagia, Anaya, and Pixie - have similar genomic architectures to mycobacteriophage TM4, a previously characterized phage that is widely used in mycobacterial genetics. The nucleotide sequence similarities warrant grouping these into Cluster K, with subdivision into three subclusters: K1, K2, and K3. Although the overall genome architectures of these phages are similar, TM4 appears to have lost at least two segments of its genome, a central region containing the integration apparatus, and a segment at the right end. This suggests that TM4 is a recent derivative of a temperate parent, resolving a long-standing conundrum about its biology, in that it was reportedly recovered from a lysogenic strain of Mycobacterium avium, but it is not capable of forming lysogens in any mycobacterial host. Like TM4, all of the Cluster K phages infect both fast- and slow-growing mycobacteria, and all of them - with the exception of TM4 - form stable lysogens in both Mycobacterium smegmatis and Mycobacterium tuberculosis; immunity assays show that all five of these phages share the same immune specificity. TM4 infects these lysogens suggesting that it was either derived from a heteroimmune temperate parent or that it has acquired a virulent phenotype. We have also characterized a widely-used conditionally replicating derivative of TM4 and identified mutations conferring the temperature-sensitive phenotype. All of the Cluster K phages contain a series of well conserved 13 bp repeats associated with the translation initiation sites of a subset of the genes; approximately one half of these contain an additional sequence feature composed of imperfectly conserved 17 bp inverted repeats separated by a variable spacer. The K1 phages integrate into the host tmRNA and the Cluster K phages represent potential new tools for the genetics of M. tuberculosis and related species. © 2011 Pope et al.

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Pope, W. H., Ferreira, C. M., Jacobs-Sera, D., Benjamin, R. C., Davis, A. J., DeJong, R. J., … Hatfull, G. F. (2011). Cluster k mycobacteriophages: Insights into the evolutionary origins of mycobacteriophage tm4. PLoS ONE, 6(10). https://doi.org/10.1371/journal.pone.0026750

Cluster k mycobacteriophages: Insights into the evolutionary origins of mycobacteriophage tm4

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