Zif, the Zoocin A Immunity Factor, Is a FemABX-Like Immunity Protein with a Novel Mode of Action

Gargis, Shaw R.; Gargis, Amy S.; Heath, Harry E.; Heath, Lucie S.; LeBlanc, Paul A.; Senn, Maria M.; Berger‐Bächi, Brigitte; Simmonds, Robin S.; Sloan, Gary L.

doi:10.1128/aem.01011-09

Cited by 18 publications

(15 citation statements)

References 29 publications

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“…Zoocin A has two functional domains, an N-terminal catalytic domain and a C-terminal substrate-binding or target recognition domain [ 43 , 44 ]. Zoocin A has been determined to act as a ᴅ-alanyl- l -alanine endopeptidase which hydrolyses the cross bridge of peptidoglycan of certain Streptococcus species [ 45 ]. Utilization of peptidoglycan hydrolases for both peptidoglycan rearrangement and pathogenicity in host cells has been described in several bacteria.…”

Section: Discussionmentioning

confidence: 99%

Identification of CiaR Regulated Genes That Promote Group B Streptococcal Virulence and Interaction with Brain Endothelial Cells

Cutting

Rosario

et al. 2016

PLoS ONE

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Group B Streptococcus (GBS) is a major causative agent of neonatal meningitis due to its ability to efficiently cross the blood-brain barrier (BBB) and enter the central nervous system (CNS). It has been demonstrated that GBS can invade human brain microvascular endothelial cells (hBMEC), a primary component of the BBB; however, the mechanism of intracellular survival and trafficking is unclear. We previously identified a two component regulatory system, CiaR/H, which promotes GBS intracellular survival in hBMEC. Here we show that a GBS strain deficient in the response regulator, CiaR, localized more frequently with Rab5, Rab7 and LAMP1 positive vesicles. Further, lysosomes isolated from hBMEC contained fewer viable bacteria following initial infection with the ΔciaR mutant compared to the WT strain. To characterize the contribution of CiaR-regulated genes, we constructed isogenic mutant strains lacking the two most down-regulated genes in the CiaR-deficient mutant, SAN_2180 and SAN_0039. These genes contributed to bacterial uptake and intracellular survival. Furthermore, competition experiments in mice showed that WT GBS had a significant survival advantage over the Δ2180 and Δ0039 mutants in the bloodstream and brain.

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Section: Discussionmentioning

confidence: 99%

Identification of CiaR Regulated Genes That Promote Group B Streptococcal Virulence and Interaction with Brain Endothelial Cells

Cutting

Rosario

et al. 2016

PLoS ONE

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“…The cross bridge in peptidoglycan of S. equi is an L-Ala-L-Ala peptide and is susceptible to the peptidoglycan hydrolase activity of zoocin A (57). Zif, an immunity factor of zoocin A, belongs to the FemABX-like protein family (58). It additively increases L-Ala residues in the cross bridges of peptidoglycans and converts L-Ala-L-Ala into L-Ala-L-Ala-L-Ala, resulting in resistance to zoocin A activity.…”

Section: Discussionmentioning

confidence: 99%

Bacteriocin Protein BacL₁of Enterococcus faecalis Targets Cell Division Loci and Specifically Recognizes l-Ala₂-Cross-Bridged Peptidoglycan

et al. 2014

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c Bacteriocin 41 (Bac41) is produced from clinical isolates of Enterococcus faecalis and consists of two extracellular proteins, BacL 1 and BacA. We previously reported that BacL 1 protein (595 amino acids, 64.5 kDa) is a bacteriolytic peptidoglycan D-isoglutamyl-L-lysine endopeptidase that induces cell lysis of E. faecalis when an accessory factor, BacA, is copresent. However, the target of BacL 1 remains unknown. In this study, we investigated the targeting specificity of BacL 1 . Fluorescence microscopy analysis using fluorescent dye-conjugated recombinant protein demonstrated that BacL 1 specifically localized at the cell divisionassociated site, including the equatorial ring, division septum, and nascent cell wall, on the cell surface of target E. faecalis cells. E nterococcus faecalis is a commensal Gram-positive bacterium in the intestinal tract of healthy humans or animals and is also known to be an opportunistic pathogen causing various infectious diseases, including urinary infectious disease, bacteremia, infective endocarditis, and others (1-3). The infection-derived E. faecalis strains often produce various plasmid-encoded bacteriocins (4, 5).Bacteriocins are bacterial peptides or proteins with antimicrobial activities (6). Heat-and acid-stable bacteriocin peptides produced by Gram-positive bacteria are divided into class I and class II according to posttranslational modifications (7,8). Class I bacteriocins are lantibiotics that contain nonproteinogenic amino acids generated by posttranslational modification (9). Only two class I bacteriocins have been identified in enterococci: ␤-hemolysin/bacteriocin (cytolysin) and enterocin W (10-14). In contrast, most enterococcal bacteriocins belong to class II and are nonmodified antimicrobial peptides, such as AS-48, enterocin A, and others (7, 15, 16). We have found the enterococcal class II bacteriocins, including Bac21, Bac31, Bac32, Bac43, and Bac51, in clinical strains of E. faecalis or Enterococcus faecium (17-21). Unlike the low-molecular-weight peptide-type class I and II bacteriocins, heat-labile antimicrobial proteins are referred to as bacteriolysins, previously named class III bacteriocins, and show enzymatic bactericidal activity (22,23). In enterococci, the bacteriolysins enterolysin A and bacteriocin 41 (Bac41) have been identified (24-26).Bac41 was originally found expressed from the pheromoneresponsive plasmid pYI14 carried by the clinical strain E. faecalis YI14 (26,27). The Bac41-type bacteriocins were also found in the E. faecalis VanB-type vancomycin-resistant E. faecalis (VRE) outbreak strains (27). Bac41 is specifically active only against E. faecalis (26, 28). The determinant region of Bac41 contains six open reading frames (ORFs), including bacL 1 , bacL 2 , bacA, and bacI (Fig. 1A). The bactericidal activity of Bac41 is actually expressed by the two extracellular components, the bacL 1 -and bacA-encoded proteins BacL 1 and BacA (26). BacL 1 and BacA are secreted proteins that coordinately exert bactericidal activity against E. faeca...

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“…In the S. equi strains carrying the zooA gene, the gene is always accompanied by a neighboring immunity gene termed zif. The zif gene product protects the zoocin A producer strain by inserting an extra alanine residue in the peptidoglycan cross bridges of its cell wall (11). There is no zif immunity gene flanking the S. agalactiae zooA gene, suggesting that the two zoocin A homologues carry out different biological functions in their respective species.…”

Section: Discussionmentioning

confidence: 99%

LytF, a Novel Competence-Regulated Murein Hydrolase in the Genus Streptococcus

2012

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Streptococcus pneumoniae and probably most other members of the genus Streptococcus are competent for natural genetic transformation. During the competent state, S. pneumoniae produces a murein hydrolase, CbpD, that kills and lyses noncompetent pneumococci and closely related species. Previous studies have shown that CbpD is essential for efficient transfer of genomic DNA from noncompetent to competent cells in vitro. Consequently, it has been proposed that CbpD together with the cognate immunity protein ComM constitutes a DNA acquisition mechanism that enables competent pneumococci to capture homologous DNA from closely related streptococci sharing the same habitat. Although genes encoding CbpD homologs or CbpD-related proteins are present in many different streptococcal species, the genomes of a number of streptococci do not encode CbpD-type proteins. In the present study we show that the genomes of nearly all species lacking CbpD encode an unrelated competence-regulated murein hydrolase termed LytF. Using Streptococcus gordonii as a model system, we obtained evidence indicating that LytF is a functional analogue of CbpD. In sum, our results show that a murein hydrolase gene is part of the competence regulon of most or all streptococcal species, demonstrating that these muralytic enzymes constitute an essential part of the streptococcal natural transformation system.

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Zif, the Zoocin A Immunity Factor, Is a FemABX-Like Immunity Protein with a Novel Mode of Action

Cited by 18 publications

References 29 publications

Identification of CiaR Regulated Genes That Promote Group B Streptococcal Virulence and Interaction with Brain Endothelial Cells

Identification of CiaR Regulated Genes That Promote Group B Streptococcal Virulence and Interaction with Brain Endothelial Cells

Bacteriocin Protein BacL₁of Enterococcus faecalis Targets Cell Division Loci and Specifically Recognizes l-Ala₂-Cross-Bridged Peptidoglycan

LytF, a Novel Competence-Regulated Murein Hydrolase in the Genus Streptococcus

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Zif, the Zoocin A Immunity Factor, Is a FemABX-Like Immunity Protein with a Novel Mode of Action

Cited by 18 publications

References 29 publications

Identification of CiaR Regulated Genes That Promote Group B Streptococcal Virulence and Interaction with Brain Endothelial Cells

Identification of CiaR Regulated Genes That Promote Group B Streptococcal Virulence and Interaction with Brain Endothelial Cells

Bacteriocin Protein BacL1of Enterococcus faecalis Targets Cell Division Loci and Specifically Recognizes l-Ala2-Cross-Bridged Peptidoglycan

LytF, a Novel Competence-Regulated Murein Hydrolase in the Genus Streptococcus

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Bacteriocin Protein BacL₁of Enterococcus faecalis Targets Cell Division Loci and Specifically Recognizes l-Ala₂-Cross-Bridged Peptidoglycan