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      Evolutionary interpretations of mycobacteriophage biodiversity and host-range through the analysis of codon usage bias

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          Abstract

          In an genomics course sponsored by the Howard Hughes Medical Institute (HHMI), undergraduate students have isolated and sequenced the genomes of more than 1,150 mycobacteriophages, creating the largest database of sequenced bacteriophages able to infect a single host, Mycobacterium smegmatis, a soil bacterium. Genomic analysis indicates that these mycobacteriophages can be grouped into 26 clusters based on genetic similarity. These clusters span a continuum of genetic diversity, with extensive genomic mosaicism among phages in different clusters. However, little is known regarding the primary hosts of these mycobacteriophages in their natural habitats, nor of their broader host ranges. As such, it is possible that the primary host of many newly isolated mycobacteriophages is not M. smegmatis, but instead a range of closely related bacterial species. However, determining mycobacteriophage host range presents difficulties associated with mycobacterial cultivability, pathogenicity and growth. Another way to gain insight into mycobacteriophage host range and ecology is through bioinformatic analysis of their genomic sequences. To this end, we examined the correlations between the codon usage biases of 199 different mycobacteriophages and those of several fully sequenced mycobacterial species in order to gain insight into the natural host range of these mycobacteriophages. We find that UPGMA clustering tends to match, but not consistently, clustering by shared nucleotide sequence identify. In addition, analysis of GC content, tRNA usage and correlations between mycobacteriophage and mycobacterial codon usage bias suggests that the preferred host of many clustered mycobacteriophages is not M. smegmatis but other, as yet unknown, members of the mycobacteria complex or closely allied bacterial species.

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          Most cited references50

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          The diversity and biogeography of soil bacterial communities.

          For centuries, biologists have studied patterns of plant and animal diversity at continental scales. Until recently, similar studies were impossible for microorganisms, arguably the most diverse and abundant group of organisms on Earth. Here, we present a continental-scale description of soil bacterial communities and the environmental factors influencing their biodiversity. We collected 98 soil samples from across North and South America and used a ribosomal DNA-fingerprinting method to compare bacterial community composition and diversity quantitatively across sites. Bacterial diversity was unrelated to site temperature, latitude, and other variables that typically predict plant and animal diversity, and community composition was largely independent of geographic distance. The diversity and richness of soil bacterial communities differed by ecosystem type, and these differences could largely be explained by soil pH (r(2) = 0.70 and r(2) = 0.58, respectively; P < 0.0001 in both cases). Bacterial diversity was highest in neutral soils and lower in acidic soils, with soils from the Peruvian Amazon the most acidic and least diverse in our study. Our results suggest that microbial biogeography is controlled primarily by edaphic variables and differs fundamentally from the biogeography of "macro" organisms.
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            tRNAscan-SE: A Program for Improved Detection of Transfer RNA Genes in Genomic Sequence

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              The codon Adaptation Index--a measure of directional synonymous codon usage bias, and its potential applications.

              P. Sharp, W Li (1987)
              A simple, effective measure of synonymous codon usage bias, the Codon Adaptation Index, is detailed. The index uses a reference set of highly expressed genes from a species to assess the relative merits of each codon, and a score for a gene is calculated from the frequency of use of all codons in that gene. The index assesses the extent to which selection has been effective in moulding the pattern of codon usage. In that respect it is useful for predicting the level of expression of a gene, for assessing the adaptation of viral genes to their hosts, and for making comparisons of codon usage in different organisms. The index may also give an approximate indication of the likely success of heterologous gene expression.
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                Author and article information

                Journal
                Microb Genom
                MGen
                Microbial Genomics
                Microbiology Society
                2057-5858
                October 2016
                21 October 2016
                : 2
                : 10
                : e000079
                Affiliations
                [ 1]Biology Department, Queens College , Queens, NY 11367, USA
                [ 2]Biology PhD Program, The Graduate Center of the City University of New York , New York, NY 10016, USA
                Author notes
                Correspondence John J. Dennehy ( john.dennehy@ 123456qc.cuny.edu )

                All supporting data, code and protocols have been provided within the article or through supplementary data files.

                Article
                mgen000079
                10.1099/mgen.0.000079
                5359403
                28348827
                20c7611b-faee-47a1-b431-1a7a0055a2f9
                © 2016 The Authors

                This is an open access article under the terms of the Creative Commons Attribution 4.0 International License, which permits unrestricted use, distribution and reproduction in any medium, provided the original author and source are credited.

                History
                : 22 April 2016
                : 18 July 2016
                Funding
                Funded by: Division of Molecular and Cellular Biosciences
                Award ID: 0918199
                Funded by: Division of Environmental Biology
                Award ID: 1148879
                Funded by: Queens College Undergraduate Research/Mentoring Education Award
                Funded by: Louis Stokes Alliance for Minority Participation in Science Technology, Engineering and Mathematics
                Funded by: Howard Hughes Medical Institute
                Award ID: SEA PHAGES Program
                Categories
                Research Paper
                Systems Microbiology
                Large-Scale Comparative Genomics
                Custom metadata
                0

                bacteriophages,codon bias,host range,mycobacteria,upgma clustering,viral trnas

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