Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties

Streptomyces diastatochromogenes Tü6028 is known to produce the polyketide antibiotic polyketomycin. The deletion of the pokOIV oxygenase gene led to a non-polyketomycin-producing mutant. Instead, novel compounds were produced by the mutant, which have not been detected before in the wild type strai...

Descripción completa

Detalles Bibliográficos
Autores principales: Greule, Anja, Marolt, Marija, Deubel, Denise, Peintner, Iris, Zhang, Songya, Jessen-Trefzer, Claudia, De Ford, Christian, Burschel, Sabrina, Li, Shu-Ming, Friedrich, Thorsten, Merfort, Irmgard, Lüdeke, Steffen, Bisel, Philippe, Müller, Michael, Paululat, Thomas, Bechthold, Andreas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2017
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5318452/
https://www.ncbi.nlm.nih.gov/pubmed/28270798
http://dx.doi.org/10.3389/fmicb.2017.00221
_version_ 1782509191240351744
author Greule, Anja
Marolt, Marija
Deubel, Denise
Peintner, Iris
Zhang, Songya
Jessen-Trefzer, Claudia
De Ford, Christian
Burschel, Sabrina
Li, Shu-Ming
Friedrich, Thorsten
Merfort, Irmgard
Lüdeke, Steffen
Bisel, Philippe
Müller, Michael
Paululat, Thomas
Bechthold, Andreas
author_facet Greule, Anja
Marolt, Marija
Deubel, Denise
Peintner, Iris
Zhang, Songya
Jessen-Trefzer, Claudia
De Ford, Christian
Burschel, Sabrina
Li, Shu-Ming
Friedrich, Thorsten
Merfort, Irmgard
Lüdeke, Steffen
Bisel, Philippe
Müller, Michael
Paululat, Thomas
Bechthold, Andreas
author_sort Greule, Anja
collection PubMed
description Streptomyces diastatochromogenes Tü6028 is known to produce the polyketide antibiotic polyketomycin. The deletion of the pokOIV oxygenase gene led to a non-polyketomycin-producing mutant. Instead, novel compounds were produced by the mutant, which have not been detected before in the wild type strain. Four different compounds were identified and named foxicins A–D. Foxicin A was isolated and its structure was elucidated as an unusual nitrogen-containing quinone derivative using various spectroscopic methods. Through genome mining, the foxicin biosynthetic gene cluster was identified in the draft genome sequence of S. diastatochromogenes. The cluster spans 57 kb and encodes three PKS type I modules, one NRPS module and 41 additional enzymes. A foxBII gene-inactivated mutant of S. diastatochromogenes Tü6028 ΔpokOIV is unable to produce foxicins. Homologous fox biosynthetic gene clusters were found in more than 20 additional Streptomyces strains, overall in about 2.6% of all sequenced Streptomyces genomes. However, the production of foxicin-like compounds in these strains has never been described indicating that the clusters are expressed at a very low level or are silent under fermentation conditions. Foxicin A acts as a siderophore through interacting with ferric ions. Furthermore, it is a weak inhibitor of the Escherichia coli aerobic respiratory chain and shows moderate antibiotic activity. The wide distribution of the cluster and the various properties of the compound indicate a major role of foxicins in Streptomyces strains.
format Online
Article
Text
id pubmed-5318452
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-53184522017-03-07 Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties Greule, Anja Marolt, Marija Deubel, Denise Peintner, Iris Zhang, Songya Jessen-Trefzer, Claudia De Ford, Christian Burschel, Sabrina Li, Shu-Ming Friedrich, Thorsten Merfort, Irmgard Lüdeke, Steffen Bisel, Philippe Müller, Michael Paululat, Thomas Bechthold, Andreas Front Microbiol Microbiology Streptomyces diastatochromogenes Tü6028 is known to produce the polyketide antibiotic polyketomycin. The deletion of the pokOIV oxygenase gene led to a non-polyketomycin-producing mutant. Instead, novel compounds were produced by the mutant, which have not been detected before in the wild type strain. Four different compounds were identified and named foxicins A–D. Foxicin A was isolated and its structure was elucidated as an unusual nitrogen-containing quinone derivative using various spectroscopic methods. Through genome mining, the foxicin biosynthetic gene cluster was identified in the draft genome sequence of S. diastatochromogenes. The cluster spans 57 kb and encodes three PKS type I modules, one NRPS module and 41 additional enzymes. A foxBII gene-inactivated mutant of S. diastatochromogenes Tü6028 ΔpokOIV is unable to produce foxicins. Homologous fox biosynthetic gene clusters were found in more than 20 additional Streptomyces strains, overall in about 2.6% of all sequenced Streptomyces genomes. However, the production of foxicin-like compounds in these strains has never been described indicating that the clusters are expressed at a very low level or are silent under fermentation conditions. Foxicin A acts as a siderophore through interacting with ferric ions. Furthermore, it is a weak inhibitor of the Escherichia coli aerobic respiratory chain and shows moderate antibiotic activity. The wide distribution of the cluster and the various properties of the compound indicate a major role of foxicins in Streptomyces strains. Frontiers Media S.A. 2017-02-21 /pmc/articles/PMC5318452/ /pubmed/28270798 http://dx.doi.org/10.3389/fmicb.2017.00221 Text en Copyright © 2017 Greule, Marolt, Deubel, Peintner, Zhang, Jessen-Trefzer, De Ford, Burschel, Li, Friedrich, Merfort, Lüdeke, Bisel, Müller, Paululat and Bechthold. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Greule, Anja
Marolt, Marija
Deubel, Denise
Peintner, Iris
Zhang, Songya
Jessen-Trefzer, Claudia
De Ford, Christian
Burschel, Sabrina
Li, Shu-Ming
Friedrich, Thorsten
Merfort, Irmgard
Lüdeke, Steffen
Bisel, Philippe
Müller, Michael
Paululat, Thomas
Bechthold, Andreas
Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties
title Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties
title_full Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties
title_fullStr Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties
title_full_unstemmed Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties
title_short Wide Distribution of Foxicin Biosynthetic Gene Clusters in Streptomyces Strains – An Unusual Secondary Metabolite with Various Properties
title_sort wide distribution of foxicin biosynthetic gene clusters in streptomyces strains – an unusual secondary metabolite with various properties
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5318452/
https://www.ncbi.nlm.nih.gov/pubmed/28270798
http://dx.doi.org/10.3389/fmicb.2017.00221
work_keys_str_mv AT greuleanja widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT maroltmarija widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT deubeldenise widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT peintneriris widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT zhangsongya widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT jessentrefzerclaudia widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT defordchristian widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT burschelsabrina widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT lishuming widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT friedrichthorsten widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT merfortirmgard widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT ludekesteffen widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT biselphilippe widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT mullermichael widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT paululatthomas widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties
AT bechtholdandreas widedistributionoffoxicinbiosyntheticgeneclustersinstreptomycesstrainsanunusualsecondarymetabolitewithvariousproperties

Ejemplares similares