The UspA1 Protein and a Second Type of UspA2 Protein Mediate Adherence of
            <i>Moraxella catarrhalis</i>
            to Human Epithelial Cells In Vitro

Lafontaine, Eric R.; Cope, Leslie D.; Aebi, Christoph; Latimer, Jo L.; McCracken, George H.; Hansen, Eric J.

doi:10.1128/jb.182.5.1364-1373.2000

Cited by 156 publications

(230 citation statements)

References 48 publications

(24 reference statements)

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“…Bioinformatic analysis of BCAM0224 predicts that this protein is an orthologue of the surface-attached collagen-binding protein YadA from Yersinia species, the best characterized member of the TAAs (Tamm et al, 1993;Koretke et al, 2006). Other members of this class, namely NadA from Neisseria meningitidis (Comanducci et al, 2002), UspA-1 and -2 from Moraxella catarrhalis (Lafontaine et al, 2000) and BadA from Bartonella henselae (Riess et al, 2004) are important pathogenicity factors, playing critical roles in processes such as bacterial adherence, biofilm formation, serum resistance and invasion of host cells (Linke et al, 2006). They represent one of the major families of surfaceexposed proteins in Gram-negative bacteria and are organized in a modular fashion, i.e.…”

Section: Discussionmentioning

confidence: 99%

Genome-wide analysis of DNA repeats in Burkholderia cenocepacia J2315 identifies a novel adhesin-like gene unique to epidemic-associated strains of the ET-12 lineage

2010

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Members of the Burkholderia cepacia complex (Bcc) are respiratory pathogens in patients with cystic fibrosis (CF). Close repetitive DNA sequences often associate with surface antigens to promote genetic variability in pathogenic bacteria. The genome of Burkholderia cenocepacia J2315, a CF isolate belonging to the epidemic lineage Edinburgh-Toronto (ET-12), was analysed for the presence of close repetitive DNA sequences. Among the 422 DNA close repeats, 45 genes potentially involved in virulence were identified and grouped into 12 classes; of these, 13 genes were included in the antigens class. Two trimeric autotransporter adhesins (TAA) among the 13 putative antigens are absent from the other Burkholderia genomes and are clustered downstream of the cci island that is a marker for transmissible B. cenocepacia strains. This cluster contains four adhesins, one outer-membrane protein, one sensor histidine kinase and two transcriptional regulators. By using PCR, we analysed three genes among 47 Bcc isolates to determine whether the cluster was conserved. These three genes were present in the isolates of the ET-12 lineage but absent in all the other members. Furthermore, the BCAM0224 gene was exclusively detected in this epidemic lineage and may serve as a valuable new addition to the field of Bcc diagnostics. The BCAM0224 gene encodes a putative TAA that demonstrates adhesive properties to the extracellular matrix protein collagen type I. Quantitative real-time PCR analysis indicated that BCAM0224 gene expression occurred preferentially for cells grown under high osmolarity, oxygen-limited conditions and oxidative stress. Inactivation of BCAM0224 in B. cenocepacia attenuates the ability of the mutant to promote cell adherence in vitro and impairs the overall bacterial virulence against Galleria mellonella as a model of infection. Together, our data show that BCAM0224 from B. cenocepacia J2315 represents a new collagen-binding TAA with no bacterial orthologues which has an important role in cellular adhesion and virulence.

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Section: Discussionmentioning

confidence: 99%

Genome-wide analysis of DNA repeats in Burkholderia cenocepacia J2315 identifies a novel adhesin-like gene unique to epidemic-associated strains of the ET-12 lineage

2010

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“…One distinct class of adhesins are the trimeric autotransporter adhesins (TAAs) (2,3), also referred to as type Vc secretion systems (4). TAAs are important virulence factors of many well-studied pathogens: Examples include YadA of Yersinia enterocolitica, a species causing enteritis, mesenteric lymphadenitis, and reactive arthritis (5); NadA of Neisseria meningitidis (6), an agent of meningitis and sepsis; BadA of Bartonella henselae (7), which is the agent of cat scratch disease; UspA1 and A2 of Moraxella catarrhalis (8), a prominent species in respiratory tract infections, and Hia of Haemophilus influenza (9), an organism causing meningitis and respiratory tract infections. Despite their role in the context of unrelated diseases, these TAAs always fulfill similar functions-adhesion to host cells, autoagglutination, and biofilm formation (3).…”

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confidence: 99%

Complete fiber structures of complex trimeric autotransporter adhesins conserved in enterobacteria

Hartmann

Grin

Dunin-Horkawicz

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Trimeric autotransporter adhesins (TAAs) are modular, highly repetitive surface proteins that mediate adhesion to host cells in a broad range of Gram-negative pathogens. Although their sizes may differ by more than one order of magnitude, they all follow the same basic head-stalk-anchor architecture, where the head mediates adhesion and autoagglutination, the stalk projects the head from the bacterial surface, and the anchor provides the export function and attaches the adhesin to the bacterial outer membrane after export is complete. In complex adhesins, head and stalk domains may alternate several times before the anchor is reached. Despite extensive sequence divergence, the structures of TAA domains are highly constrained, due to the tight interleaving of their constituent polypeptide chains. We have therefore taken a "domain dictionary" approach to characterize representatives for each domain type by X-ray crystallography and use these structures to reconstruct complete TAA fibers. With SadA from Salmonella enterica, EhaG from enteropathogenic Escherichia coli (EHEC), and UpaG from uropathogenic E. coli (UPEC), we present three representative structures of a complex adhesin that occur in a conserved genomic context in Enterobacteria and is essential in the infection process of uropathogenic E. coli. Our work proves the applicability of the dictionary approach to understanding the structure of a class of proteins that are otherwise poorly tractable by high-resolution methods and provides a basis for the rapid and detailed annotation of newly identified TAAs.coiled coil | β-layer

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“…The hybrid UspA2H consists of UspA1 and UspA2 with its N-terminal (head region) and C-terminal (near-end stalk and membrane-anchored region) having shared sequence similarity with UspA1 and UspA2, respectively (17,19,20). The stalk region is highly conserved between UspA1, UspA2, and UspA2H of different strains (17,19,21). The UspAs bind the extracellular matrix proteins laminin and fibronectin and are essential for attachment of M. catarrhalis to epithelial cells (17,(22)(23)(24), and they play important roles in M. catarrhalis serum resistance by interacting with C3, C4b-binding protein (C4BP), and vitronectin (25)(26)(27)(28).…”

mentioning

confidence: 99%

“…UspA1 and UspA2 are multifunctional proteins, have highly conserved epitopes, and thus are of considerable interest as potential vaccine candidates (9,18). The hybrid UspA2H consists of UspA1 and UspA2 with its N-terminal (head region) and C-terminal (near-end stalk and membrane-anchored region) having shared sequence similarity with UspA1 and UspA2, respectively (17,19,20). The stalk region is highly conserved between UspA1, UspA2, and UspA2H of different strains (17,19,21).…”

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confidence: 99%

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Immune Evasion ofMoraxella catarrhalisInvolves Ubiquitous Surface Protein A-Dependent C3d Binding

Hallström

Nordström

Tan

et al. 2011

The Journal of Immunology

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The complement system plays an important role in eliminating invading pathogens. Activation of complement results in C3b deposition (opsonization), phagocytosis, anaphylatoxin (C3a, C5a) release, and consequently cell lysis. Moraxella catarrhalis is a human respiratory pathogen commonly found in children with otitis media and in adults with chronic obstructive pulmonary disease. The species has evolved multiple complement evasion strategies, which among others involves the ubiquitous surface protein (Usp) family consisting of UspA1, A2, and A2 hybrid. In the present study, we found that the ability of M. catarrhalis to bind C3 correlated with UspA expression and that C3 binding contributed to serum resistance in a large number of clinical isolates. Recombinantly expressed UspA1 and A2 inhibit both the alternative and classical pathways, C3b deposition, and C3a generation when bound to the C3 molecule. We also revealed that the M. catarrhalis UspA-binding domain on C3b was located to C3d and that the major bacterial C3d-binding domains were within UspA1299–452 and UspA2165–318. The interaction with C3 was not species specific since UspA-expressing M. catarrhalis also bound mouse C3 that resulted in inhibition of the alternative pathway of mouse complement. Taken together, the binding of C3 to UspAs is an efficient strategy of Moraxella to block the activation of complement and to inhibit C3a-mediated inflammation.

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The UspA1 Protein and a Second Type of UspA2 Protein Mediate Adherence of Moraxella catarrhalis to Human Epithelial Cells In Vitro

Cited by 156 publications

References 48 publications

Genome-wide analysis of DNA repeats in Burkholderia cenocepacia J2315 identifies a novel adhesin-like gene unique to epidemic-associated strains of the ET-12 lineage

Genome-wide analysis of DNA repeats in Burkholderia cenocepacia J2315 identifies a novel adhesin-like gene unique to epidemic-associated strains of the ET-12 lineage

Complete fiber structures of complex trimeric autotransporter adhesins conserved in enterobacteria

Immune Evasion ofMoraxella catarrhalisInvolves Ubiquitous Surface Protein A-Dependent C3d Binding

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