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Publication : C/EBPβ Promotes Immunity to Oral Candidiasis through Regulation of β-Defensins.

First Author  Simpson-Abelson MR Year  2015
Journal  PLoS One Volume  10
Issue  8 Pages  e0136538
PubMed ID  26317211 Mgi Jnum  J:243022
Mgi Id  MGI:5907430 Doi  10.1371/journal.pone.0136538
Citation  Simpson-Abelson MR, et al. (2015) C/EBPbeta Promotes Immunity to Oral Candidiasis through Regulation of beta-Defensins. PLoS One 10(8):e0136538
abstractText  Humans or mice subjected to immunosuppression, such as corticosteroids or anti-cytokine biologic therapies, are susceptible to mucosal infections by the commensal fungus Candida albicans. Recently it has become evident that the Th17/IL-17 axis is essential for immunity to candidiasis, but the downstream events that control immunity to this fungus are poorly understood. The CCAAT/Enhancer Binding Protein-beta (C/EBPbeta) transcription factor is important for signaling by multiple inflammatory stimuli, including IL-17. C/EBPbeta is regulated in a variety of ways by IL-17, and controls several downstream IL-17 target genes. However, the role of C/EBPbeta in vivo is poorly understood, in part because C/EBPbeta-deficient mice are challenging to breed and work with. In this study, we sought to understand the role of C/EBPbeta in the context of an IL-17-dependent immune response, using C. albicans infection as a model system. Confirming prior findings, we found that C/EBPbeta is required for immunity to systemic candidiasis. In contrast, C/EBPbeta(-/-) mice were resistant to oropharyngeal candidiasis (OPC), in a manner indistinguishable from immunocompetent WT mice. However, C/EBPbeta(-/-) mice experienced more severe OPC than WT mice in the context of cortisone-induced immunosuppression. Expression of the antimicrobial peptide beta-defensin (BD)-3 correlated strongly with susceptibility in C/EBPbeta(-/-) mice, but no other IL-17-dependent genes were associated with susceptibility. Therefore, C/EBPbeta contributes to immunity to mucosal candidiasis during cortisone immunosuppression in a manner linked to beta-defensin 3 expression, but is apparently dispensable for the IL-17-dependent response.
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