Pore-forming pyocin S5 utilizes the FptA ferripyochelin receptor to kill Pseudomonas aeruginosa

Elfarash, Ameer; Dingemans, Jozef; Ye, Lumeng; Hassan, A. Amir; Craggs, M.; Reimmann, Cornelia; Thomas, Mark S.; Cornélis, Pierre

doi:10.1099/mic.0.070672-0

Cited by 53 publications

(64 citation statements)

References 36 publications

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“…It typically concerns outer membrane proteins (OMPs) involved in the uptake of iron via siderophores: type I ferripyoverdine transporter FpvAI for pyocins S2, S4, and SD2 (17–19), type II ferripyoverdine transporter FpvAII for pyocin S3 (20), and ferripyochelin receptor FptA for pyocin S5 (21). Some S pyocins carry (almost) identical amino-terminal regions and basically differ only in their toxin-immunity module, emphasizing the peculiar modularity of these allelopathic molecules.…”

Section: Introductionmentioning

confidence: 99%

A Natural ChimericPseudomonasBacteriocin with Novel Pore-Forming Activity Parasitizes the Ferrichrome Transporter

Ghequire

Kemland

Anoz-Carbonell

et al. 2017

mBio

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Modular bacteriocins represent a major group of secreted protein toxins with a narrow spectrum of activity, involved in interference competition between Gram-negative bacteria. These antibacterial proteins include a domain for binding to the target cell and a toxin module at the carboxy terminus. Self-inhibition of producers is provided by coexpression of linked immunity genes that transiently inhibit the toxin’s activity through formation of bacteriocin-immunity complexes or by insertion in the inner membrane, depending on the type of toxin module. We demonstrate strain-specific inhibitory activity for PmnH, a Pseudomonas bacteriocin with an unprecedented dual-toxin architecture, hosting both a colicin M domain, potentially interfering with peptidoglycan synthesis, and a novel colicin N-type domain, a pore-forming module distinct from the colicin Ia-type domain in Pseudomonas aeruginosa pyocin S5. A downstream-linked gene product confers PmnH immunity upon susceptible strains. This protein, ImnH, has a transmembrane topology similar to that of Pseudomonas colicin M-like and pore-forming immunity proteins, although homology with either of these is essentially absent. The enhanced killing activity of PmnH under iron-limited growth conditions reflects parasitism of the ferrichrome-type transporter for entry into target cells, a strategy shown here to be used as well by monodomain colicin M-like bacteriocins from pseudomonads. The integration of a second type of toxin module in a bacteriocin gene could offer a competitive advantage against bacteria displaying immunity against only one of both toxic activities.

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Section: Introductionmentioning

confidence: 99%

A Natural ChimericPseudomonasBacteriocin with Novel Pore-Forming Activity Parasitizes the Ferrichrome Transporter

Ghequire

Kemland

Anoz-Carbonell

et al. 2017

mBio

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“…E-type colicins parasitize the vitamin B 12 receptor, BtuB, as their primary receptor in the outer membrane [9] and the Tol-Pal complex in the periplasm [5]. S-type pyocins S2 and S5 bind FpvA and FptA, respectively, which import siderophore-chelated iron [10,11]. How they translocate across the outer membrane is not known, although pyocin AP41, the receptor of which has yet to be identified, may translocate into cells via the Tol-Pal system [12].…”

Section: Introductionmentioning

confidence: 99%

Structural and biophysical analysis of nuclease protein antibiotics

Klein

Wojdyla

Joshi

et al. 2016

Biochemical Journal

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Protein antibiotics (bacteriocins) are a large and diverse family of multidomain toxins that kill specific Gram-negative bacteria during intraspecies competition for resources. Our understanding of the mechanism of import of such potent toxins has increased significantly in recent years, especially with the reporting of several structures of bacteriocin domains. Less well understood is the structural biochemistry of intact bacteriocins and how these compare across bacterial species. Here, we focus on endonuclease (DNase) bacteriocins that target the genomes of Escherichia coli and Pseudomonas aeruginosa, known as E-type colicins and S-type pyocins, respectively, bound to their specific immunity (Im) proteins. First, we report the 3.2 Å structure of the DNase colicin ColE9 in complex with its ultra-high affinity Im protein, Im9. In contrast with Im3, which when bound to the ribonuclease domain of the homologous colicin ColE3 makes contact with the translocation (T) domain of the toxin, we find that Im9 makes no such contact and only interactions with the ColE9 cytotoxic domain are observed. Second, we report small-angle X-ray scattering data for two S-type DNase pyocins, S2 and AP41, into which are fitted recently determined X-ray structures for isolated domains. We find that DNase pyocins and colicins are both highly elongated molecules, even though the order of their constituent domains differs. We discuss the implications of these architectural similarities and differences in the context of the translocation mechanism of protein antibiotics through the cell envelope of Gram-negative bacteria.

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“…Bakkal et al (2010) have reported that bacteriocins produced by Pseudomonas and Burkholderia strains have intra-and interspecies bacteriocin-like inhibition ability within the CF lung (Bakkal et al, 2010). Some of these bacteriocins, such as the Pseudomonas pyocin, share the same receptors as siderophores (Denayer et al, 2007;Elfarash et al, 2014) and therefore interfere with iron acquisition of their target host. It has also been demonstrated that P. aeruginosa can lyse Staphylococcus aureus using PqsA, a coenzyme ligase, to gain access to internalized iron (Mashburn et al, 2005).…”

Section: Pathogen Interactions and Competition For Iron In Cfmentioning

confidence: 99%

Iron acquisition in the cystic fibrosis lung and potential for novel therapeutic strategies

Tyrrell¹,

Callaghan²

2016

Microbiology

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Iron acquisition is vital to microbial survival and is implicated in the virulence of many of the pathogens that reside in the cystic fibrosis (CF) lung. The multifaceted nature of iron acquisition by both bacterial and fungal pathogens encompasses a range of conserved and speciesspecific mechanisms, including secretion of iron-binding siderophores, utilization of siderophores from other species, release of iron from host iron-binding proteins and haemoproteins, and ferrous iron uptake. Pathogens adapt and deploy specific systems depending on iron availability, bioavailability of the iron pool, stage of infection and presence of competing pathogens. Understanding the dynamics of pathogen iron acquisition has the potential to unveil new avenues for therapeutic intervention to treat both acute and chronic CF infections. Here, we examine the range of strategies utilized by the primary CF pathogens to acquire iron and discuss the different approaches to targeting iron acquisition systems as an antimicrobial strategy.

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Pore-forming pyocin S5 utilizes the FptA ferripyochelin receptor to kill Pseudomonas aeruginosa

Cited by 53 publications

References 36 publications

A Natural ChimericPseudomonasBacteriocin with Novel Pore-Forming Activity Parasitizes the Ferrichrome Transporter

A Natural ChimericPseudomonasBacteriocin with Novel Pore-Forming Activity Parasitizes the Ferrichrome Transporter

Structural and biophysical analysis of nuclease protein antibiotics

Iron acquisition in the cystic fibrosis lung and potential for novel therapeutic strategies

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