Protection against systemic candidiasis in mice immunized with secreted aspartic proteinase 2

Vilanova, Manuel; Teixeira, Luzia; Caramalho, Íris; Torrado, Egídio; Marques, António; Madureira, Pedro; Ribeiro, Ana M.; Ferreira, Paula; Gama, Miguel; Demengeot, Jocelyne

doi:10.1111/j.1365-2567.2004.01819.x

Cited by 64 publications

(57 citation statements)

References 57 publications

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“…These results are consistent with those of earlier studies in which anti-enolase antibodies were found to be partially protective in experimental SC (88,89) and supports the notion that other protective mechanisms against SC are also implicated (13)(14)(15)90).…”

Section: Serum Anti-bgl2p Igg Antibodies Are a Novel Independent Diagsupporting

confidence: 83%

“…Research efforts currently focus on screening both for Candida cell wall polysaccharides (mannans or ␤-1,3-glucans), extracellular proteins (secreted aspartyl proteinase), cytoplasmic proteins (enolase or heat shock protein 90), metabolites (D-arabinitol), or nucleic acids (DNA or RNA) and for anti-Candida antibodies in body fluids of SC patients (11)(12)(13)(14)(15). The relevance of well defined Candida cell wall proteins or their related antibodies in SC diagnosis, prognosis, and therapy, however, has been barely examined (16 -18).…”

Section: Not Only Does Systemic Candidiasis (Sc)mentioning

confidence: 99%

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Decoding Serological Response to Candida Cell Wall Immunome into Novel Diagnostic, Prognostic, and Therapeutic Candidates for Systemic Candidiasis by Proteomic and Bioinformatic Analyses

Pitarch

Jiménez

Nombela

et al. 2006

Molecular & Cellular Proteomics

129

123

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In an effort to bring novel diagnostic and prognostic biomarkers or even potential targets for vaccine design for systemic candidiasis (SC) into the open, a systematic proteomic approach coupled with bioinformatic analysis was used to decode the serological response to Candida wall immunome in SC patients. Serum levels of IgG antibodies against Candida wall-associated proteins (proteins secreted from protoplasts in active wall regeneration, separated by two-dimensional gel electrophoresis, and identified by mass spectrometry) were measured in 45 SC patients, 57 non-SC patients, and 61 healthy subjects by Western blotting. Two-way hierarchical clustering and principal component analysis of their serum anti-Candida wall antibody expression patterns discriminated SC patients from controls and highlighted the heterogeneity of their expression profiles. Multivariate logistic regression models demonstrated that high levels of antibodies against glucan 1,3-␤-glucosidase (Bgl2p) and the antiwall phosphoglycerate kinase antibody seropositivity were the only independent predictors of SC. Receiver operating characteristic curve analysis revealed no difference between their combined evaluation and measurement of anti-Bgl2p antibodies alone. In a logistic regression model adjusted for known prognostic factors for mortality, SC patients with high anti-Bgl2p antibody levels or a positive anti-wall enolase antibody status, which correlated with each other, had a reduced 2-month risk of death. After controlling for each other, only the seropositivity for anti-wall enolase antibodies was an independent predictor of a lower risk of fatality, supporting that these mediated the protective effect. No association between serum anti-cytoplasmic enolase antibody levels and outcomes was established, suggesting a specific mechanism of enolase processing during wall biogenesis. We conclude that serum anti-Bgl2p antibodies are a novel accurate diagnostic biomarker for SC and that, at high levels,

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Section: Serum Anti-bgl2p Igg Antibodies Are a Novel Independent Diagsupporting

confidence: 83%

Section: Not Only Does Systemic Candidiasis (Sc)mentioning

confidence: 99%

Decoding Serological Response to Candida Cell Wall Immunome into Novel Diagnostic, Prognostic, and Therapeutic Candidates for Systemic Candidiasis by Proteomic and Bioinformatic Analyses

Pitarch

Jiménez

Nombela

et al. 2006

Molecular & Cellular Proteomics

129

123

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“…Although the secretion of aspartic proteases has long been recognized as a virulence-associated trait of Candida spp. (38), the vaccinating potential of secreted proteases from Candida (37), and now from Aspergillus, further adds to the biological functions of proteases at the fungus/host interface, as already suggested (39). In this regard, we have recently shown a crucial role for host protease-activated receptors in murine aspergillosis (39).…”

Section: Discussionmentioning

confidence: 89%

Immune Sensing of Aspergillus fumigatus Proteins, Glycolipids, and Polysaccharides and the Impact on Th Immunity and Vaccination

Bozza

Clavaud

Giovannini

et al. 2009

The Journal of Immunology

164

186

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The ability of the fungus Aspergillus fumigatus to activate, suppress, or subvert host immune response during life cycle in vivo through dynamic changing of cell wall structure and secretion implicates discriminative immune sensing of distinct fungal components. In this study, we have comparatively assessed secreted- and membrane-anchored proteins, glycolipids, and polysaccharides for the ability to induce vaccine-dependent protection in transplanted mice and Th cytokine production by human-specific CD4+ T cell clones. The results show that the different fungal components are endowed with the distinct capacity to activate Th cell responses in mice and humans, with secreted proteins inducing Th2 cell activation, membrane proteins Th1/Treg, glycolipids Th17, and polysaccharides mostly IL-10 production. Of interest, the side-by-side comparison revealed that at least three fungal components (a protease and two glycosylphosphatidylinositol-anchored proteins) retained their immunodominant Th1/Treg activating potential from mice to humans. This suggests that the broadness and specificity of human T cell repertoire against the fungus could be selectively exploited with defined immunoactive Aspergillus Ags.

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“…Different structural microbial Ags such as LPS or the staphylococcal protein A are known to induce polyclonal B cell activation. In addition, several microbial extracellular proteins including enzymes have also been described as B cell activators (8,13,25,51,52). The ability of microbial constituents to induce polyclonal B cell activation in the infected host constitutes a mechanism of host immune evasion used by pathogens to suppress the specific, potentially protective, immune responses (5,14,21).…”

Section: Discussionmentioning

confidence: 99%

“…Previous reports showing that immunization against a particular VIP confers protection against the infection caused by the VIP-producing microbe, further indicates the important role of VIP for the success of microbial colonization (11,(22)(23)(24)(25).…”

mentioning

confidence: 99%

Streptococcus agalactiae GAPDH Is a Virulence-Associated Immunomodulatory Protein

Madureira¹,

Baptista

Vieira

et al. 2007

The Journal of Immunology

Self Cite

125

109

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Certain extracellular proteins produced by several pathogenic microorganisms interfere with the host immune system facilitating microbial colonization and were thus designated virulence-associated immunomodulatory proteins. In this study, a protein with B lymphocyte stimulatory activity was isolated from culture supernatants of Streptococcus agalactiae strain NEM316. This protein, with an apparent molecular mass of 45 kDa, was identified as GAPDH by N-terminal amino acid sequencing. The gapC gene was cloned and expressed in Escherichia coli for the production of a recombinant histidyl-tagged protein. The recombinant GAPDH (rGAPDH), purified in an enzymatically active form, induced in vitro an up-regulation of CD69 expression on B cells from normal and BCR transgenic mice. In addition, rGAPDH induced an increase in the numbers of total, but not of rGAPDH-specific, splenic Ig-secreting cells in C57BL/6 mice treated i.p. with this protein. These in vitro- and in vivo-elicited B cell responses suggest that the B cell stimulatory effect of rGAPDH is independent of BCR specificity. A S. agalactiae strain overexpressing GAPDH showed increased virulence as compared with the wild-type strain in C57BL/6 mice. This virulence was markedly reduced in IL-10-deficient and anti-rGAPDH antiserum-treated mice. These results suggest that IL-10 production, which was detected at higher concentrations in the serum of rGAPDH-treated mice, is important in determining the successfulness of the host colonization by S. agalactiae and they highlight the direct role of GAPDH in this process. Taken together, our data demonstrate that S. agalactiae GAPDH is a virulence-associated immunomodulatory protein.

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Protection against systemic candidiasis in mice immunized with secreted aspartic proteinase 2

Cited by 64 publications

References 57 publications

Decoding Serological Response to Candida Cell Wall Immunome into Novel Diagnostic, Prognostic, and Therapeutic Candidates for Systemic Candidiasis by Proteomic and Bioinformatic Analyses

Decoding Serological Response to Candida Cell Wall Immunome into Novel Diagnostic, Prognostic, and Therapeutic Candidates for Systemic Candidiasis by Proteomic and Bioinformatic Analyses

Immune Sensing of Aspergillus fumigatus Proteins, Glycolipids, and Polysaccharides and the Impact on Th Immunity and Vaccination

Streptococcus agalactiae GAPDH Is a Virulence-Associated Immunomodulatory Protein

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