Abstract
Response regulators are a critical part of the two-component system of gene expression regulation in bacteria, transferring a signal from a sensor kinase into DNA binding activity resulting in alteration of gene expression. In this study, we investigated a previously uncharacterized response regulator in Francisella novicida, FTN_1452 that we have named BfpR (Biofilm-regulating Francisella protein Regulator, FTN_1452). In contrast to another Francisella response regulator, QseB/PmrA, BfpR appears to be a negative regulator of biofilm production, and also a positive regulator of antimicrobial peptide resistance in this bacterium. The protein was crystallized and X-ray crystallography studies produced a 1.8 Å structure of the BfpR N-terminal receiver domain revealing interesting insight into its potential interaction with the sensor kinase. Structural analysis of BfpR places it in the OmpR/PhoP family of bacterial response regulators along with WalR and ResD. Proteomic and transcriptomic analyses suggest that BfpR overexpression affects expression of the critical Francisella virulence factor iglC, as well as other proteins in the bacterium. We demonstrate that mutation of bfpR is associated with an antimicrobial peptide resistance phenotype, a phenotype also associated with other response regulators, for the human cathelicidin peptide LL-37 and a sheep antimicrobial peptide SMAP-29. F. novicida with mutated bfpR replicated better than WT in intracellular infection assays in human-derived macrophages suggesting that the down-regulation of iglC expression in bfpR mutant may enable this intracellular replication to occur. Response regulators have been shown to play important roles in the regulation of bacterial biofilm production. We demonstrate that F. novicida biofilm formation was highly increased in the bfpR mutant, corresponding to altered glycogen synthesis. Waxworm infection experiments suggest a role of BfpR as a negative modulator of iglC expression with de-repression by Mg2+. In this study, we find that the response regulator BfpR may be a negative regulator of biofilm formation, and a positive regulator of antimicrobial peptide resistance in F. novicida.
Highlights
Francisella are Gram-negative, fastidious bacteria found primarily in the Northern Hemisphere
Cases of tularemia in the United States are rare and recently increasing, and interest in Francisella-related research is high (Dennis et al, 2001; Oyston et al, 2004). This is due to recent outbreaks of tularemia around the world and the fact that F. tularensis is classified as a Category A Biological threat Agent
We previously investigated the role of the response regulator QseB/PmrA (FTN_1465) in biofilm formation in F. novicida (Durham-Colleran et al, 2010; van Hoek, 2013), and demonstrated that biofilm formation is dependent on both the orphan response regulator (QseB/PrmA) and the orphan sensor kinase (QseC, FTN_1617)
Summary
Francisella are Gram-negative, fastidious bacteria found primarily in the Northern Hemisphere. F. tularensis Schu S4, the highly infectious humanvirulent Type A strain, encodes two sensor kinase genes, two FIGURE 1 | Two component systems annotated or predicted in Francisella species. The fully virulent F. tularensis Schu S4 genome is annotated to contain two sensor histidine kinases and two response regulators, none of which are within intact (paired) two component systems. The two component system genes previously identified in F. tularensis Schu S4 include two sensor kinases FTT_0094c (qseC) and FTT_1736c (kdpD) and two response regulators FTT_1543 (bfpR) and FTT_1557c (qseB/pmrA), all of which are considered to be “orphan” or not paired in a canonical two component system operon. We previously investigated the role of the response regulator QseB/PmrA (FTN_1465) in biofilm formation in F. novicida (Durham-Colleran et al, 2010; van Hoek, 2013), and demonstrated that biofilm formation is dependent on both the orphan response regulator (QseB/PrmA) and the orphan sensor kinase (QseC, FTN_1617). Our findings led us to identify a role of BfpR within F. novicida including resistance to AMPs and biofilm formation
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