Functional Analysis of the Alternative Sigma-28 Factor FliA and Its Anti-Sigma Factor FlgM of the Nonflagellated Legionella Species L. oakridgensis

Hana Tlapák; Kerstin Rydzewski; Tino Schulz; Dennis Weschka; Eva Schunder; Klaus Heuner

doi:10.1128/JB.00018-17

Functional Analysis of the Alternative Sigma-28 Factor FliA and Its Anti-Sigma Factor FlgM of the Nonflagellated Legionella Species L. oakridgensis

J Bacteriol. 2017 May 9;199(11):e00018-17. doi: 10.1128/JB.00018-17. Print 2017 Jun 1.

Authors

Hana Tlapák¹, Kerstin Rydzewski¹, Tino Schulz², Dennis Weschka¹, Eva Schunder², Klaus Heuner³

Affiliations

¹ Cellular Interactions of Bacterial Pathogens, ZBS 2, Robert Koch Institute, Berlin, Germany.
² University Tissue Bank, Institute of Transfusion Medicine, Charité-Universitätsmedizin, Berlin, Germany.
³ Cellular Interactions of Bacterial Pathogens, ZBS 2, Robert Koch Institute, Berlin, Germany heunerk@rki.de.

Abstract

Legionella oakridgensis causes Legionnaires' disease but is known to be less virulent than Legionella pneumophilaL. oakridgensis is one of the Legionella species that is nonflagellated. The genes of the flagellar regulon are absent, except those encoding the alternative sigma-28 factor (FliA) and its anti-sigma-28 factor (FlgM). Similar to L. oakridgensis, Legionella adelaidensis and Legionella londiniensis, located in the same phylogenetic clade, have no flagellar regulon, although both are positive for fliA and flgM Here, we investigated the role and function of both genes to better understand the role of FliA, the positive regulator of flagellin expression, in nonflagellated strains. We demonstrated that the FliA gene of L. oakridgensis encodes a functional sigma-28 factor that enables the transcription start from the sigma-28-dependent promoter site. The investigations have shown that FliA is necessary for full fitness of L. oakridgensis Interestingly, expression of FliA-dependent genes depends on the growth phase and temperature, as already shown for L. pneumophila strains that are flagellated. In addition, we demonstrated that FlgM is a negative regulator of FliA-dependent gene expression. FlgM seems to be degraded in a growth-phase- and temperature-dependent manner, instead of being exported into the medium as reported for most bacteria. The degradation of FlgM leads to an increase of FliA activity.IMPORTANCE A less virulent Legionella species, L. oakridgensis, causes Legionnaires' disease and is known to not have flagella, even though L. oakridgensis has the regulator of flagellin expression (FliA). This protein has been shown to be involved in the expression of virulence factors. Thus, the strain was chosen for use in this investigation to search for FliA target genes and to identify putative virulence factors of L. oakridgensis One of the five major target genes of FliA identified here encodes the anti-FliA sigma factor FlgM. Interestingly, in contrast to most homologs in other bacteria, FlgM in L. oakridgensis seems not to be transported from the cell so that FliA gets activated. In L. oakridgensis, FlgM seems to be degraded by protease activities.

Keywords: FlgM; FliA; Legionella oakridgensis; anti-sigma factor; flagella; sigma-28 factor.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amino Acid Sequence
Bacterial Proteins / chemistry
Bacterial Proteins / genetics
Bacterial Proteins / metabolism*
Flagella / genetics
Flagella / metabolism
Gene Expression Regulation, Bacterial*
Legionella / chemistry
Legionella / genetics
Legionella / metabolism*
Phylogeny
Regulon
Sequence Alignment
Sigma Factor / chemistry
Sigma Factor / genetics
Sigma Factor / metabolism*

Substances

Bacterial Proteins
FliA protein, Bacteria
Sigma Factor
FlgM protein, Bacteria