Sulfonium Acids Loaded onto an Unusual Thiotemplate Assembly Line Construct the Cyclopropanol Warhead of a Burkholderia Virulence Factor

Publikation: Beitrag in FachzeitschriftKurzmitteilungForschungPeer-Review

Autoren

  • Felix Trottmann
  • Keishi Ishida
  • Jakob Franke
  • Aleksa Stanišić
  • Mie Ishida-Ito
  • Hajo Kries
  • Georg Pohnert
  • Christian Hertweck

Organisationseinheiten

Externe Organisationen

  • Leibniz-Institut für Naturstoff-Forschung und Infektionsbiologie e. V.Hans-Knöll-Institut
  • Friedrich-Schiller-Universität Jena
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Details

OriginalspracheEnglisch
Seiten (von - bis)13511-13515
Seitenumfang5
FachzeitschriftAngewandte Chemie - International Edition
Jahrgang59
Ausgabenummer32
Frühes Online-Datum21 Apr. 2020
PublikationsstatusVeröffentlicht - 3 Aug. 2020

Abstract

Pathogenic bacteria of the Burkholderia pseudomallei group cause severe infectious diseases such as glanders and melioidosis. Malleicyprols were identified as important bacterial virulence factors, yet the biosynthetic origin of their cyclopropanol warhead has remained enigmatic. By a combination of mutational analysis and metabolomics we found that sulfonium acids, dimethylsulfoniumpropionate (DMSP) and gonyol, known as osmolytes and as crucial components in the global organosulfur cycle, are key intermediates en route to the cyclopropanol unit. Functional genetics and in vitro analyses uncover a specialized pathway to DMSP involving a rare prokaryotic SET-domain methyltransferase for a cryptic methylation, and show that DMSP is loaded onto the NRPS-PKS hybrid assembly line by an adenylation domain dedicated to zwitterionic starter units. Then, the megasynthase transforms DMSP into gonyol, as demonstrated by heterologous pathway reconstitution in E. coli.

ASJC Scopus Sachgebiete

Ziele für nachhaltige Entwicklung

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Sulfonium Acids Loaded onto an Unusual Thiotemplate Assembly Line Construct the Cyclopropanol Warhead of a Burkholderia Virulence Factor. / Trottmann, Felix; Ishida, Keishi; Franke, Jakob et al.
in: Angewandte Chemie - International Edition, Jahrgang 59, Nr. 32, 03.08.2020, S. 13511-13515.

Publikation: Beitrag in FachzeitschriftKurzmitteilungForschungPeer-Review

Trottmann F, Ishida K, Franke J, Stanišić A, Ishida-Ito M, Kries H et al. Sulfonium Acids Loaded onto an Unusual Thiotemplate Assembly Line Construct the Cyclopropanol Warhead of a Burkholderia Virulence Factor. Angewandte Chemie - International Edition. 2020 Aug 3;59(32):13511-13515. Epub 2020 Apr 21. doi: 10.1002/anie.202003958, 10.1002/ange.202003958, 10.15488/11039
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title = "Sulfonium Acids Loaded onto an Unusual Thiotemplate Assembly Line Construct the Cyclopropanol Warhead of a Burkholderia Virulence Factor",
abstract = "Pathogenic bacteria of the Burkholderia pseudomallei group cause severe infectious diseases such as glanders and melioidosis. Malleicyprols were identified as important bacterial virulence factors, yet the biosynthetic origin of their cyclopropanol warhead has remained enigmatic. By a combination of mutational analysis and metabolomics we found that sulfonium acids, dimethylsulfoniumpropionate (DMSP) and gonyol, known as osmolytes and as crucial components in the global organosulfur cycle, are key intermediates en route to the cyclopropanol unit. Functional genetics and in vitro analyses uncover a specialized pathway to DMSP involving a rare prokaryotic SET-domain methyltransferase for a cryptic methylation, and show that DMSP is loaded onto the NRPS-PKS hybrid assembly line by an adenylation domain dedicated to zwitterionic starter units. Then, the megasynthase transforms DMSP into gonyol, as demonstrated by heterologous pathway reconstitution in E. coli.",
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note = "Funding Information: We thank A. Perner for LC‐MS measurements. Financial support by the DFG (SFB 1127 ChemBioSys, and Leibniz Award to C.H.) and the European Regional Development Fund (ERDF) (MassNat) is gratefully acknowledged. J.F. acknowledges financial support by the SMART BIOTECS alliance between the Technische Universit{\"a}t Braunschweig and the Leibniz Universit{\"a}t Hannover, supported by the Ministry of Science and Culture (MWK) of Lower Saxony, Germany. H.K. received a fellowship from the Daimler and Benz foundation. ",
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AU - Trottmann, Felix

AU - Ishida, Keishi

AU - Franke, Jakob

AU - Stanišić, Aleksa

AU - Ishida-Ito, Mie

AU - Kries, Hajo

AU - Pohnert, Georg

AU - Hertweck, Christian

N1 - Funding Information: We thank A. Perner for LC‐MS measurements. Financial support by the DFG (SFB 1127 ChemBioSys, and Leibniz Award to C.H.) and the European Regional Development Fund (ERDF) (MassNat) is gratefully acknowledged. J.F. acknowledges financial support by the SMART BIOTECS alliance between the Technische Universität Braunschweig and the Leibniz Universität Hannover, supported by the Ministry of Science and Culture (MWK) of Lower Saxony, Germany. H.K. received a fellowship from the Daimler and Benz foundation.

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N2 - Pathogenic bacteria of the Burkholderia pseudomallei group cause severe infectious diseases such as glanders and melioidosis. Malleicyprols were identified as important bacterial virulence factors, yet the biosynthetic origin of their cyclopropanol warhead has remained enigmatic. By a combination of mutational analysis and metabolomics we found that sulfonium acids, dimethylsulfoniumpropionate (DMSP) and gonyol, known as osmolytes and as crucial components in the global organosulfur cycle, are key intermediates en route to the cyclopropanol unit. Functional genetics and in vitro analyses uncover a specialized pathway to DMSP involving a rare prokaryotic SET-domain methyltransferase for a cryptic methylation, and show that DMSP is loaded onto the NRPS-PKS hybrid assembly line by an adenylation domain dedicated to zwitterionic starter units. Then, the megasynthase transforms DMSP into gonyol, as demonstrated by heterologous pathway reconstitution in E. coli.

AB - Pathogenic bacteria of the Burkholderia pseudomallei group cause severe infectious diseases such as glanders and melioidosis. Malleicyprols were identified as important bacterial virulence factors, yet the biosynthetic origin of their cyclopropanol warhead has remained enigmatic. By a combination of mutational analysis and metabolomics we found that sulfonium acids, dimethylsulfoniumpropionate (DMSP) and gonyol, known as osmolytes and as crucial components in the global organosulfur cycle, are key intermediates en route to the cyclopropanol unit. Functional genetics and in vitro analyses uncover a specialized pathway to DMSP involving a rare prokaryotic SET-domain methyltransferase for a cryptic methylation, and show that DMSP is loaded onto the NRPS-PKS hybrid assembly line by an adenylation domain dedicated to zwitterionic starter units. Then, the megasynthase transforms DMSP into gonyol, as demonstrated by heterologous pathway reconstitution in E. coli.

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