Galactosylation of the Secondary Cell Wall Polysaccharide of Bacillus anthracis and Its Contribution to Anthrax Pathogenesis

Château, Alice; Lunderberg, Justin Mark; Oh, Seung Keun; Abshire, Teresa G.; Friedlander, Arthur M.; Quinn, Conrad P.; Missiakas, Dominique; Schneewind, Olaf

doi:10.1128/jb.00562-17

Cited by 15 publications

(24 citation statements)

References 58 publications

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“…In P. alvei , the SCWP consists of pyruvylated [→3)-β- D -Man p NAc-(1→4)-β- D -Glc p NAc-(1→] disaccharide repeats ( Schäffer and Messner, 2005 ; Janesch et al, 2013a ). The SCWP repeats of B. anthracis ( Mesnage et al, 2000 ; Forsberg et al, 2012 ) and B. cereus strains ( Choudhury et al, 2006 ; Forsberg et al, 2011 ) as analyzed from hydrofluoric acid-treated material are extensions of the disaccharide motif by one α- D -GlcNAc residue yielding [→4)-β- D -Man p NAc-(1→4)-β- D -Glc p NAc-(1→6)-α- D -Glc p NAc-(1→] and include additional non-stoichiometric galactosyl ( Chateau et al, 2018 ) and acetyl modifications; in these SCWPs, exclusively the non-reducing-end β- D -ManNAc residue carries a 4,6-linked pyruvate ketal modification.…”

Section: Discussionmentioning

confidence: 99%

Functional Characterization of Enzymatic Steps Involved in Pyruvylation of Bacterial Secondary Cell Wall Polymer Fragments

et al. 2018

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Various mechanisms of protein cell surface display have evolved during bacterial evolution. Several Gram-positive bacteria employ S-layer homology (SLH) domain-mediated sorting of cell-surface proteins and concomitantly engage a pyruvylated secondary cell-wall polymer as a cell-wall ligand. Specifically, pyruvate ketal linked to β-D-ManNAc is regarded as an indispensable epitope in this cell-surface display mechanism. That secondary cell wall polymer (SCWP) pyruvylation and SLH domain-containing proteins are functionally coupled is supported by the presence of an ortholog of the predicted pyruvyltransferase CsaB in bacterial genomes, such as those of Bacillus anthracis and Paenibacillus alvei. The P. alvei SCWP, consisting of pyruvylated disaccharide repeats [→4)-β-D-GlcNAc-(1→3)-4,6-Pyr-β-D-ManNAc-(1→] serves as a model to investigate the widely unexplored pyruvylation reaction. Here, we reconstituted the underlying enzymatic pathway in vitro in combination with synthesized compounds, used mass spectrometry, and nuclear magnetic resonance spectroscopy for product characterization, and found that CsaB-catalyzed pyruvylation of β-D-ManNAc occurs at the stage of the lipid-linked repeat. We produced the P. alvei TagA (PAV_RS07420) and CsaB (PAV_RS07425) enzymes as recombinant, tagged proteins, and using a synthetic 11-phenoxyundecyl-diphosphoryl-α-GlcNAc acceptor, we uncovered that TagA is an inverting UDP-α-D-ManNAc:GlcNAc-lipid carrier transferase, and that CsaB is a pyruvyltransferase, with synthetic UDP-α-D-ManNAc and phosphoenolpyruvate serving as donor substrates. Next, to substitute for the UDP-α-D-ManNAc substrate, the recombinant UDP-GlcNAc-2-epimerase MnaA (PAV_RS07610) of P. alvei was included in this in vitro reconstitution system. When all three enzymes, their substrates and the lipid-linked GlcNAc primer were combined in a one-pot reaction, a lipid-linked SCWP repeat precursor analog was obtained. This work highlights the biochemical basis of SCWP biosynthesis and bacterial pyruvyl transfer.

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Section: Discussionmentioning

confidence: 99%

Functional Characterization of Enzymatic Steps Involved in Pyruvylation of Bacterial Secondary Cell Wall Polymer Fragments

et al. 2018

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“…Depletion of the glycosyltransferases results in irregularly shaped non-viable cells (132). In addition, a mutant lacking a UDP-glucose 4-epimerase required for SCWP galactosylation exhibits reduced encapsulation and decreased virulence in a murine model for anthrax (133). Recent investigations of B. cereus isolates causing anthrax-like disease indicate SCWP with structure similar to that of B. anthracis , but with an additional α-Gal substitution at O3 of ManNAc (134).…”

Section: Cell Structure and Developmentmentioning

confidence: 99%

The Bacillus cereus Group: Bacillus Species with Pathogenic Potential

2019

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The “Bacillus cereus group” includes several Bacillus species with closely related phylogeny. The most well-studied members of the group, Bacillus anthracis, B. cereus, and B. thuringiensis are known for their pathogenic potential. Here we present the historical rationale for speciation and discuss shared and unique features of these bacteria. Aspects of cell morphology and physiology, and genome sequence similarity and gene synteny support close evolutionary relationships for these three species. For many strains, distinct differences in virulence factor synthesis provide facile means for species assignment. B. anthracis is the causative agent of anthrax. Some B. cereus strains are commonly recognized as food poisoning agents, but strains can also cause localized wound and eye infections as well as systemic disease. Certain B. thuringiensis strains are entomopathogens and have been commercialized for use as biopesticides, while some strains have been reported to cause infection in immunocompromised individuals. In this chapter we compare and contrast B. anthracis, B. cereus, and B. thuringiensis, including ecology, cell structure and development, virulence attributes, gene regulation and genetic exchange systems, and experimental models of disease.

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“…The S-layer gene cluster [99,112,113,114] encodes, among others, components for pyruvylation ( B. anthracis CsaB) and O -acetylation of the terminal SCWP trisaccharide, and a Wzy-like protein. The other gene clusters play predicted roles in the formation of lipid-linked precursors of the murein linkage unit and the trisaccharide repeat [112,114,115,116]. The SCWP biosynthesis model proposes the separate assembly of different undp-PP-linked building blocks in the cytoplasm—the murein linkage unit, trisaccharide repeat, and terminal modified trisaccharide [113]—followed by the individual translocation across the cytoplasmic membrane via Wzx, followed by SCWP polymerization at the outer face of the membrane involving Wzy [113].…”

Section: Ketal-pyruvylated Glycoconjugatesmentioning

confidence: 99%

Pyruvate Substitutions on Glycoconjugates

Hager

Sützl

Stefanović

et al. 2019

IJMS

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Glycoconjugates are the most diverse biomolecules of life. Mostly located at the cell surface, they translate into cell-specific “barcodes” and offer a vast repertoire of functions, including support of cellular physiology, lifestyle, and pathogenicity. Functions can be fine-tuned by non-carbohydrate modifications on the constituting monosaccharides. Among these modifications is pyruvylation, which is present either in enol or ketal form. The most commonly best-understood example of pyruvylation is enol-pyruvylation of N-acetylglucosamine, which occurs at an early stage in the biosynthesis of the bacterial cell wall component peptidoglycan. Ketal-pyruvylation, in contrast, is present in diverse classes of glycoconjugates, from bacteria to algae to yeast—but not in humans. Mild purification strategies preventing the loss of the acid-labile ketal-pyruvyl group have led to a collection of elucidated pyruvylated glycan structures. However, knowledge of involved pyruvyltransferases creating a ring structure on various monosaccharides is scarce, mainly due to the lack of knowledge of fingerprint motifs of these enzymes and the unavailability of genome sequences of the organisms undergoing pyruvylation. This review compiles the current information on the widespread but under-investigated ketal-pyruvylation of monosaccharides, starting with different classes of pyruvylated glycoconjugates and associated functions, leading to pyruvyltransferases, their specificity and sequence space, and insight into pyruvate analytics.

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Galactosylation of the Secondary Cell Wall Polysaccharide of Bacillus anthracis and Its Contribution to Anthrax Pathogenesis

Cited by 15 publications

References 58 publications

Functional Characterization of Enzymatic Steps Involved in Pyruvylation of Bacterial Secondary Cell Wall Polymer Fragments

Functional Characterization of Enzymatic Steps Involved in Pyruvylation of Bacterial Secondary Cell Wall Polymer Fragments

The Bacillus cereus Group: Bacillus Species with Pathogenic Potential

Pyruvate Substitutions on Glycoconjugates

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