| Literature DB >> 28878118 |
Alyssa N Nylander1,2,3, Gerald D Ponath1, Pierre-Paul Axisa1,3, Mayyan Mubarak1, Mary Tomayko4, Vijay K Kuchroo5, David Pitt1, David A Hafler1,2,3.
Abstract
Recent data indicate that there are different subpopulations of Th17 cells that can express a regulatory as opposed to an inflammatory gene signature. The transmembrane glycoprotein PDPN is critical in the development of multiple organs including the lymphatic system and has been described on T cells in mouse models of autoimmune Th17 inflammation. Here, we demonstrate that unlike in mice, PDPN+ T cells induced under classic Th17-polarizing conditions express transcription factors associated with Th17 cells but do not produce IL-17. Moreover, these cells express a transcriptional profile enriched for immunosuppressive and regulatory pathways and express a distinct cytokine profile compared with potentially pathogenic PDPN- Th17 cells. Ligation of PDPN by its ligand CLEC-2 ameliorates the Th17 inflammatory response. IL-17 secretion is restored with shRNA gene silencing of PDPN. Furthermore, PDPN expression is reduced via an Sgk1-mediated pathway under proinflammatory, high sodium chloride conditions. Finally, CD3+PDPN+ T cells are devoid of IL-17 in skin biopsies from patients with candidiasis, a prototypical Th17-driven skin disease. Thus, our data support the hypothesis that PDPN may serve as a marker of a nonpathogenic Th17 cell subset and may also functionally regulate pathogenic Th17 inflammation.Entities:
Keywords: Autoimmunity; Cytokines; Fungal infections; Immunology; T cells
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Year: 2017 PMID: 28878118 PMCID: PMC5621890 DOI: 10.1172/jci.insight.92321
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708