Introduction. Candidiasis remains a notable health problem in subjects with underlying disease and several risk factors (diabetes, deep surgery, HIV infection, genetic predisposition and others) because of elevated mortality (candidemia and deep-seated infections), chronicity and recurrences in high prevalence clinical settings (oral and vaginal candidiasis), perceived increased risk of drug-resistance and lack of specific preventive measures such as vaccines. Within this framework, the high capacity of the major agent of candidiasis, Candida albicans (C. albicans), to express virulence factors causing inflammation and deceiving host immune system is remarkable and should constitute an important new concept/target to fight candidiasis by new tools providing an alternative or integration to the existing drugs. Secretory aspartyl-proteinases of C. albicans (SAP) are dominant virulence attributes of C. albicans and are considered to play an important role in the pathogenicity of this fungus. Materials and Methods. Using purified, enzymatically active, recombinant SAP, we demonstrated by western blot and flow cytometry analysis that SAP, including SAP2 and SAP6, are strong activators of NLRP3 inflammasome both in monocytes and epithelial cells. Results. The inflammasome response occurs via NLRP3 and caspase-1 activation which cleaves pro-IL1beta into secreted bioactive IL-1beta. The demonstration that proinflammatory cytokine production is induced by SAP through inflammasome activation implies new role for these virulence factors related to their structural features. Discussion and Conclusions. Particularly, inflammasome activation may contribute to severe inflammation and recruitment of neutrophils, a scenario characteristic in the pathology of vaginal candidiasis, during SAP production or exposure in the vaginal environment. Our data strongly suggest that SAP2 production may contribute to the excessive inflammatory response observed during C. albicans infections, which may be the hallmark of at least some Candida pathologies.

Secretory aspartyl-proteinases of Candida albicans contribute to severe inflammation observed in the course of vaginal candidiasis / Pericolini, Eva; E., Gabrielli; E., Roselletti; E., Luciano; S., Sabbatini; A., Vecchiarelli; A., Cassone. - In: NEW MICROBIOLOGICA. - ISSN 1121-7138. - 37:(2014). (Intervento presentato al convegno 42° National Congress of the Italian Society of Microbiology tenutosi a Turin nel 28 September- 1 October 2014).

Secretory aspartyl-proteinases of Candida albicans contribute to severe inflammation observed in the course of vaginal candidiasis

PERICOLINI, Eva;
2014

Abstract

Introduction. Candidiasis remains a notable health problem in subjects with underlying disease and several risk factors (diabetes, deep surgery, HIV infection, genetic predisposition and others) because of elevated mortality (candidemia and deep-seated infections), chronicity and recurrences in high prevalence clinical settings (oral and vaginal candidiasis), perceived increased risk of drug-resistance and lack of specific preventive measures such as vaccines. Within this framework, the high capacity of the major agent of candidiasis, Candida albicans (C. albicans), to express virulence factors causing inflammation and deceiving host immune system is remarkable and should constitute an important new concept/target to fight candidiasis by new tools providing an alternative or integration to the existing drugs. Secretory aspartyl-proteinases of C. albicans (SAP) are dominant virulence attributes of C. albicans and are considered to play an important role in the pathogenicity of this fungus. Materials and Methods. Using purified, enzymatically active, recombinant SAP, we demonstrated by western blot and flow cytometry analysis that SAP, including SAP2 and SAP6, are strong activators of NLRP3 inflammasome both in monocytes and epithelial cells. Results. The inflammasome response occurs via NLRP3 and caspase-1 activation which cleaves pro-IL1beta into secreted bioactive IL-1beta. The demonstration that proinflammatory cytokine production is induced by SAP through inflammasome activation implies new role for these virulence factors related to their structural features. Discussion and Conclusions. Particularly, inflammasome activation may contribute to severe inflammation and recruitment of neutrophils, a scenario characteristic in the pathology of vaginal candidiasis, during SAP production or exposure in the vaginal environment. Our data strongly suggest that SAP2 production may contribute to the excessive inflammatory response observed during C. albicans infections, which may be the hallmark of at least some Candida pathologies.
2014
42° National Congress of the Italian Society of Microbiology
Turin
28 September- 1 October 2014
37
Pericolini, Eva; E., Gabrielli; E., Roselletti; E., Luciano; S., Sabbatini; A., Vecchiarelli; A., Cassone
Secretory aspartyl-proteinases of Candida albicans contribute to severe inflammation observed in the course of vaginal candidiasis / Pericolini, Eva; E., Gabrielli; E., Roselletti; E., Luciano; S., Sabbatini; A., Vecchiarelli; A., Cassone. - In: NEW MICROBIOLOGICA. - ISSN 1121-7138. - 37:(2014). (Intervento presentato al convegno 42° National Congress of the Italian Society of Microbiology tenutosi a Turin nel 28 September- 1 October 2014).
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11380/1120055
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