BipA Is Associated with Preventing Autoagglutination and Promoting Biofilm Formation in Bordetella holmesii

Hiramatsu, Yukihiro; Saito, Momoko; Otsuka, Nao; Suzuki, Eri; Watanabe, Mineo; Shibayama, Keigo; Kamachi, Kazunari

doi:10.1371/journal.pone.0159999

Cited by 15 publications

(17 citation statements)

References 39 publications

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“…Since BipA is highly conserved amongst bacteria 36,37,49 it is tempting to speculate that the BipA-dependent control of biofilm formation by temperature observed in V. cholerae could be conserved in other bacteria. In agreement with this hypothesis, deletion of BipA has been associated to increased biofilm levels in P. aeruginosa PAO1 41 and Bordetella holmesii 45 . BipA from E. coli and P. aeruginosa cross-complemented V. cholerae ΔbipA temperature-dependent phenotypes (Figure 3D), further supporting a model of BipA function as a bacterial “temperature sensor”.…”

Section: Discussionsupporting

confidence: 70%

“…Mutations in BipA have been associated with a cold-sensitive phenotype in E. coli 44 , but a clean deletion of vc2744 in V. cholerae co969 did not influence growth or cell morphology at any temperature (SM Figure 3). In other bacteria, BipA has been implicated in biofilm formation 41,45,38,46 , but the mechanism behind this phenotype has remained elusive. As BipA is thought to be a ribosome-binding GTPase that regulates ribosome assembly 47 , we reasoned that VC2744 could be repressing biofilm development at low temperatures through translational regulation.…”

Section: Resultsmentioning

confidence: 99%

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A temperature-dependent translational switch controls biofilm development inVibrio cholerae

Santos

Blake

Sit

et al. 2020

Preprint

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16The gastrointestinal pathogen Vibrio cholerae frequently forms biofilms during its life 17 cycle. Biofilm formation is vital for protection against environmental stresses and is 18 thought to facilitate intestinal colonization. Adaptation to temperature is crucial for V. 19 cholerae survival, as the pathogen is exposed to seasonal temperature variations in 20 the aquatic environment, and temperature fluctuations during host-environment 21 transitions. Here, we show that V. cholerae strains naturally lacking the master biofilm 22 transcriptional regulator HapR are unable to develop colony rugosity at low 23 temperatures. We find that BipA, a ribosome-associated GTPase, accounts for this 24 temperature-dependent control of biofilm formation by repressing translation of the 25 primary biofilm transcriptional activators VpsR and VpsT at low temperatures. In vitro 26 studies demonstrate that low temperatures influence BipA structural conformation and 27 decrease its sensitivity to proteolysis. Proteomic analyses reveal that BipA exerts 28 temperature-dependent control over >200 proteins in V. cholerae involved in a 29 multitude of cell processes, including biofilm assembly. Our study reveals a 30 remarkable new facet of the complex V. cholerae biofilm regulatory cascade and 31suggests that combined transcriptional-translational control could be a common 32 mechanism by which bacteria adapt to environmental flux.A common strategy of bacteria for adaptation and survival to changing environmental 35 conditions is the formation of biofilms: bacterial communities enclosed in an 36 extracellular matrix. Vibrio cholerae, the causative agent of the severe diarrhoeal 37 disease cholera, forms biofilms both in biotic and abiotic surfaces in the aquatic 38 environment that inhabits 1-3 and also in the intestine of the human host 4,5 . The 39 formation of biofilms enhances persistence of V. cholerae, since it provides protection 40 against environmental insults, predators and stress conditions and allows a better 41 access to nutrients 3 . There is some evidence indicating that biofilm-formation capacity 42 is critical for intestinal colonization 5 and biofilms have also been linked to a 43 hyperinfectious phenotype 6 . 44V. cholerae's biofilm is primarily composed of VPS (Vibrio polysaccharide), matrix 45 proteins (RbmA, RbmC and Bap1) and extracellular DNA 7-13 . The genes encoding the 46 activities for the production of VPS, grouped in the vpsI and vpsII clusters, and the 47 genes encoding the RbmA and RbmC matrix proteins, located in the rbm cluster 48 between vpsI and vpsII clusters, form the so-called V. cholerae biofilm-matrix cluster 49 (VcBMC) 7-10 . 50 Biofilm formation inVibrio cholerae is a highly regulated process, controlled by the 51 transcriptional activators VpsR, VpsT and AphA, the transcriptional repressors HapR 52 and H-NS, small regulatory RNAs, alternative sigma factors (RpoS, RpoN and RpoE), 53 and small nucleotide signalling (c-di-GMP, cAMP, ppGpp). Specific environmental 54 signals such as changes...

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Section: Discussionsupporting

confidence: 70%

Section: Resultsmentioning

confidence: 99%

A temperature-dependent translational switch controls biofilm development inVibrio cholerae

Santos

Blake

Sit

et al. 2020

Preprint

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“…In the present study, we used a mouse intranasal challenge model, as the model is strongly correlated with the efficacy of vaccines in humans and is, so far, the sole model system that is used for in vivo studies of B. holmesii . In fact, studies of Zhang et al and the present study clearly suggested that commercial pertussis vaccines had little effect against B. holmesii .…”

Section: Discussionmentioning

confidence: 70%

“…Furthermore, BipA is not strictly required for colonization of the respiratory tract by B. pertussis but is, instead, necessary immediately before and/or after a transmission event . However, the initial level of colonization by B. holmesii strain BH2Sm r ‐ΔBipA was found to be significantly lower than that of the wild‐type strain in a murine model . Thus, the BipA‐like protein of B. holmesii might be involved in binding to the respiratory tract and might play an important role in protection of mice that have been immunized with aBH vaccine.…”

Section: Discussionmentioning

confidence: 99%

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Development of vaccines against pertussis caused by Bordetella holmesii using a mouse intranasal challenge model

Saito

Odanaka

Otsuka

et al. 2016

Microbiology and Immunology

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Bordetella holmesii is recognized as the third causative agent of pertussis (whooping cough) in addition to Bordetella pertussis and Bordetella parapertussis. Pertussis caused by B. holmesii is not rare around the world. However, to date, there is no effective vaccine against B. holmesii. We examined the protective potency of pertussis vaccines available in Japan and vaccines prepared from B. holmesii. A murine model of respiratory infection was exploited to evaluate protective potency. No Japanese commercial pertussis vaccines were effective against B. holmesii. In contrast, a wBH vaccine and an aBH vaccine prepared from B. holmesii were both protective. Passive immunization with sera from mice immunized with aBH vaccine established protection against B. holmesii, indicating that B. holmesii-specific serum antibodies might play an important role in protection. Immuno-proteomic analysis with sera from mice immunized with aBH vaccine revealed that the sera recognized a BipAlike protein of B. holmesii. An aBH vaccine prepared from a BipA-like protein-deficient mutant strain did not have a protective effect against B. holmesii. Taken together, our results suggest that the BipAlike protein plays an important role in the protective efficacy of aBH vaccine.Key words BipA-like protein, Bordetella holmesii, pertussis, whooping cough.Pertussis (whooping cough) is a highly contagious respiratory disease caused, in most cases, by Bordetella pertussis. Introduction of effective pertussis vaccines has dramatically reduced the incidence of pertussis caused by B. pertussis worldwide (1). However, current pertussis vaccines are not effective against other causative agents of pertussis, such as B. parapertussis and B. holmesii (2-5). Our previous studies showed that effective vaccines against B. parapertussis can be prepared from formalin-inactivated whole cells or FHA of B. parapertussis (3). The goal of the present study was to develop effective vaccines against respiratory infection by B. holmesii.Bordetella holmesii was first reported in 1995 after isolation from a patient with sepsis, and it is recognized as a causative agent of systemic infection, mainly in immunocompromised hosts (6). During the past decade, B. holmesii has also been isolated from patients with pertussis-like symptoms (7,8). Recent epidemiological studies suggest that pertussis caused by B. holmesii List of Abbreviations: 2D PAGE, two dimensional polyacrylamide gel electrophores; aBH, acellular vaccine prepared from Bordetella holmesii; BG agar, Bordet-Gengou agar; BH2Sm r -4BipA, BipA-like protein deficient-mutant of B. holmesii; CFU, colony-forming units; CasS/S, Stainer Scholte medium supplemented with 0.25 (w/v) Casamino acids; DPBS, Dulbecco's modified phosphate-buffered saline (À) pH 7.4; DTT, dithiothreitol; DTaP, diphtheriatetanus acellular pertussis vaccine; FHA, filamentous hemagglutinin; FIM, fimbriae; HE, hematoxylin-eosin; Incubation buffer, washing buffer containing 10% (w/v) skimmed milk; PFGE, pulse field gel electrophoresis; PRN, ...

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Microbial biofilms and their role in acute and chronic pathogenesis

Srivastava,

Kumari,

Prasad Gond

et al. 2024

Microbial Biofilms

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BipA Is Associated with Preventing Autoagglutination and Promoting Biofilm Formation in Bordetella holmesii

Cited by 15 publications

References 39 publications

A temperature-dependent translational switch controls biofilm development inVibrio cholerae

A temperature-dependent translational switch controls biofilm development inVibrio cholerae

Development of vaccines against pertussis caused by Bordetella holmesii using a mouse intranasal challenge model

Microbial biofilms and their role in acute and chronic pathogenesis

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