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  Legionella shows a diverse secondary metabolism dependent on a broad spectrum Sfp-type phosphopantetheinyl transferase

Tobias, N. J., Ahrendt, T., Schell, U., Miltenberger, M., Hilbi, H., & Bode, H. B. (2016). Legionella shows a diverse secondary metabolism dependent on a broad spectrum Sfp-type phosphopantetheinyl transferase. PEERJ, 4: e2720. doi:10.7717/peerj.2720.

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 Creators:
Tobias, Nicholas J.1, Author
Ahrendt, Tilman1, Author
Schell, Ursula1, Author
Miltenberger, Melissa1, Author
Hilbi, Hubert1, Author
Bode, Helge B.2, Author           
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1external, ou_persistent22              
2Goethe-Universität Frankfurt am Main, External Organizations, ou_421891              

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 Abstract: Several members of the genus Legionella cause Legionnaires' disease, a potentially debilitating form of pneumonia. Studies frequently focus on the abundant number of virulence factors present in this genus. However, what is often overlooked is the role of secondary metabolites from Legionella. Following whole genome sequencing, we assembled and annotated the Legionella parisiensis DSM 19216 genome. Together with 14 other members of the Legionella, we performed comparative genomics and analysed the secondary metabolite potential of each strain. We found that Legionella contains a huge variety of biosynthetic gene clusters (BGCs) that are potentially making a significant number of novel natural products with undefined function. Surprisingly, only a single Sfp-like phosphopantetheinyl transferase is found in all Legionella strains analyzed that might be responsible for the activation of all carrier proteins in primary (fatty acid biosynthesis) and secondary metabolism (polyketide and non-ribosomal peptide synthesis). Using conserved active site motifs, we predict some novel compounds that are probably involved in cell-cell communication, differing to known communication systems. We identify several gene clusters, which may represent novel signaling mechanisms and demonstrate the natural product potential of Legionella.

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 Dates: 2016
 Publication Status: Published online
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 Identifiers: ISI: 000389149700004
DOI: 10.7717/peerj.2720
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Title: PEERJ
Source Genre: Journal
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Pages: - Volume / Issue: 4 Sequence Number: e2720 Start / End Page: - Identifier: ISSN: 2167-8359