Abstract
Pseudomonas aeruginosa is a clinically relevant species involved in biofilm-based chronic infections. We provide evidence that the P. aeruginosa LapG protein functions as a periplasmic protease that can cleave the protein adhesin CdrA off the cell surface, and thereby plays a role in biofilm formation and biofilm dispersal. The P. aeruginosa LapG protein is shown to be a functional homolog of the Pseudomonas putida LapG protein which has previously been shown to function as a periplasmic protease that targets the surface adhesin LapA. Transposon mutagenesis and characterization of defined knockout mutants provided evidence that the CdrA adhesin is a target of LapG in P. aeruginosa. A wspF lapG double mutant was hyper-aggregating and hyper biofilm forming, whereas a wspF lapG cdrA triple mutant lost these phenotypes. In addition, western blot detection of CdrA in culture supernatants and whole-cell protein fractions showed that CdrA was retained in the whole-cell protein fraction when LapG was absent, whereas it was found in the culture supernatant when LapG was present. The finding that CdrA is a target of LapG in P. aeruginosa is surprising because CdrA has no homology to LapA. In this study, evidence is provided that the Pseudomonas aeruginosa LapG protein functions as a periplasmic protease that can cleave the protein adhesin CdrA off the cell surface, and thereby plays a role in biofilm formation and biofilm dispersal. Evidence for this includes the finding that a lapG mutant with high c-di-GMP content is hyper-aggregating whereas an additional deletion of cdrA results in a nonaggregating phenotype.
| Original language | English |
|---|---|
| Journal | MicrobiologyOpen |
| Volume | 4 |
| Issue number | 6 |
| Pages (from-to) | 917-930 |
| Number of pages | 14 |
| ISSN | 2045-8827 |
| DOIs | |
| Publication status | Published - 1 Dec 2015 |