[PDF][PDF] CD103+ dendritic cells control Th17 cell function in the lung

T Zelante, AYW Wong, TJ Ping, J Chen, HR Sumatoh… - Cell reports, 2015 - cell.com
T Zelante, AYW Wong, TJ Ping, J Chen, HR Sumatoh, E Viganò, YH Bing, B Lee, F Zolezzi…
Cell reports, 2015cell.com
Th17 cells express diverse functional programs while retaining their Th17 identity, in some
cases exhibiting a stem-cell-like phenotype. Whereas the importance of Th17 cell regulation
in autoimmune and infectious diseases is firmly established, the signaling pathways
controlling their plasticity are undefined. Using a mouse model of invasive pulmonary
aspergillosis, we found that lung CD103+ dendritic cells (DCs) would produce IL-2,
dependent on NFAT signaling, leading to an optimally protective Th17 response. The …
Summary
Th17 cells express diverse functional programs while retaining their Th17 identity, in some cases exhibiting a stem-cell-like phenotype. Whereas the importance of Th17 cell regulation in autoimmune and infectious diseases is firmly established, the signaling pathways controlling their plasticity are undefined. Using a mouse model of invasive pulmonary aspergillosis, we found that lung CD103+ dendritic cells (DCs) would produce IL-2, dependent on NFAT signaling, leading to an optimally protective Th17 response. The absence of IL-2 in DCs caused unrestrained production of IL-23 and fatal hyperinflammation, which was characterized by strong Th17 polarization and the emergence of a Th17 stem-cell-like population. Although several cell types may be affected by deficient IL-2 production in DCs, our findings identify the balance between IL-2 and IL-23 productions by lung DCs as an important regulator of the local inflammatory response to infection.
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