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      Antibiotic-producing symbionts dynamically transition between plant pathogenicity and insect-defensive mutualism

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          Abstract

          Pathogenic and mutualistic bacteria associated with eukaryotic hosts often lack distinctive genomic features, suggesting regular transitions between these lifestyles. Here we present evidence supporting a dynamic transition from plant pathogenicity to insect-defensive mutualism in symbiotic Burkholderia gladioli bacteria. In a group of herbivorous beetles, these symbionts protect the vulnerable egg stage against detrimental microbes. The production of a blend of antibiotics by B. gladioli, including toxoflavin, caryoynencin and two new antimicrobial compounds, the macrolide lagriene and the isothiocyanate sinapigladioside, likely mediate this defensive role. In addition to vertical transmission, these insect symbionts can be exchanged via the host plant and retain the ability to initiate systemic plant infection at the expense of the plant's fitness. Our findings provide a paradigm for the transition between pathogenic and mutualistic lifestyles and shed light on the evolution and chemical ecology of this defensive mutualism.

          Abstract

          Observations of recent or dynamic transitions between parasitism and mutualism are scarce. Here, Flórez et al. provide evidence that Burkholderia gladioli bacteria can protect the eggs of herbivorous beetles by producing antimicrobial compounds, while retaining their ancestral ability to infect plants.

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          Most cited references42

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          MRBAYES: Bayesian inference of phylogenetic trees.

          The program MRBAYES performs Bayesian inference of phylogeny using a variant of Markov chain Monte Carlo. MRBAYES, including the source code, documentation, sample data files, and an executable, is available at http://brahms.biology.rochester.edu/software.html.
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            16S ribosomal DNA amplification for phylogenetic study.

            A set of oligonucleotide primers capable of initiating enzymatic amplification (polymerase chain reaction) on a phylogenetically and taxonomically wide range of bacteria is described along with methods for their use and examples. One pair of primers is capable of amplifying nearly full-length 16S ribosomal DNA (rDNA) from many bacterial genera; the additional primers are useful for various exceptional sequences. Methods for purification of amplified material, direct sequencing, cloning, sequencing, and transcription are outlined. An obligate intracellular parasite of bovine erythrocytes, Anaplasma marginale, is used as an example; its 16S rDNA was amplified, cloned, sequenced, and phylogenetically placed. Anaplasmas are related to the genera Rickettsia and Ehrlichia. In addition, 16S rDNAs from several species were readily amplified from material found in lyophilized ampoules from the American Type Culture Collection. By use of this method, the phylogenetic study of extremely fastidious or highly pathogenic bacterial species can be carried out without the need to culture them. In theory, any gene segment for which polymerase chain reaction primer design is possible can be derived from a readily obtainable lyophilized bacterial culture.
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              Evolutionary microbial genomics: insights into bacterial host adaptation.

              Host-adapted bacteria include mutualists and pathogens of animals, plants and insects. Their study is therefore important for biotechnology, biodiversity and human health. The recent rapid expansion in bacterial genome data has provided insights into the adaptive, diversifying and reductive evolutionary processes that occur during host adaptation. The results have challenged many pre-existing concepts built from studies of laboratory bacterial strains. Furthermore, recent studies have revealed genetic changes associated with transitions from parasitism to mutualism and opened new research avenues to understand the functional reshaping of bacteria as they adapt to growth in the cytoplasm of a eukaryotic host.
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                Author and article information

                Journal
                Nat Commun
                Nat Commun
                Nature Communications
                Nature Publishing Group
                2041-1723
                28 April 2017
                2017
                : 8
                : 15172
                Affiliations
                [1 ]Insect Symbiosis Research Group, Max Planck Institute for Chemical Ecology , Hans-Knöll-Straβe 8, 07745 Jena, Germany
                [2 ]Department for Evolutionary Ecology, Institute of Organismic and Molecular Evolution, Johannes Gutenberg University , Johann-Joachim-Becher-Weg 13, 55128 Mainz, Germany
                [3 ]Department of Biomolecular Chemistry, Leibniz Institute for Natural Products Research and Infection Biology , HKI, Beutenbergstraβe 11a, 07745 Jena, Germany
                [4 ]Department of Biochemistry and Microbiology, UNESP-São Paulo State University , Av. 24A, n. 1515-Bela Vista, Rio Claro, São Paulo 13506-900, Brazil
                [5 ]Chair for Natural Product Chemistry, Friedrich Schiller University , 07743 Jena, Germany
                Author notes
                Article
                ncomms15172
                10.1038/ncomms15172
                5414355
                28452358
                486b1fb9-2b8d-4b91-b56d-3f16c63ae314
                Copyright © 2017, The Author(s)

                This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article's Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/

                History
                : 11 December 2016
                : 06 March 2017
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