Clearance of influenza virus from the lung depends on migratory langerin+CD11b− but not plasmacytoid dendritic cells
CH GeurtsvanKessel, MAM Willart, LS van Rijt… - The Journal of …, 2008 - rupress.org
CH GeurtsvanKessel, MAM Willart, LS van Rijt, F Muskens, M Kool, C Baas, K Thielemans…
The Journal of experimental medicine, 2008•rupress.orgAlthough dendritic cells (DCs) play an important role in mediating protection against
influenza virus, the precise role of lung DC subsets, such as CD11b− and CD11b+
conventional DCs or plasmacytoid DCs (pDCs), in different lung compartments is currently
unknown. Early after intranasal infection, tracheal CD11b− CD11chi DCs migrated to the
mediastinal lymph nodes (MLNs), acquiring co-stimulatory molecules in the process. This
emigration from the lung was followed by an accumulation of CD11b+ CD11chi DCs in the …
influenza virus, the precise role of lung DC subsets, such as CD11b− and CD11b+
conventional DCs or plasmacytoid DCs (pDCs), in different lung compartments is currently
unknown. Early after intranasal infection, tracheal CD11b− CD11chi DCs migrated to the
mediastinal lymph nodes (MLNs), acquiring co-stimulatory molecules in the process. This
emigration from the lung was followed by an accumulation of CD11b+ CD11chi DCs in the …
Although dendritic cells (DCs) play an important role in mediating protection against influenza virus, the precise role of lung DC subsets, such as CD11b− and CD11b+ conventional DCs or plasmacytoid DCs (pDCs), in different lung compartments is currently unknown. Early after intranasal infection, tracheal CD11b−CD11chi DCs migrated to the mediastinal lymph nodes (MLNs), acquiring co-stimulatory molecules in the process. This emigration from the lung was followed by an accumulation of CD11b+CD11chi DCs in the trachea and lung interstitium. In the MLNs, the CD11b+ DCs contained abundant viral nucleoprotein (NP), but these cells failed to present antigen to CD4 or CD8 T cells, whereas resident CD11b−CD8α+ DCs presented to CD8 cells, and migratory CD11b−CD8α− DCs presented to CD4 and CD8 T cells. When lung CD11chi DCs and macrophages or langerin+CD11b−CD11chi DCs were depleted using either CD11c–diphtheria toxin receptor (DTR) or langerin-DTR mice, the development of virus-specific CD8+ T cells was severely delayed, which correlated with increased clinical severity and a delayed viral clearance. 120G8+ CD11cint pDCs also accumulated in the lung and LNs carrying viral NP, but in their absence, there was no effect on viral clearance or clinical severity. Rather, in pDC-depleted mice, there was a reduction in antiviral antibody production after lung clearance of the virus. This suggests that multiple DCs are endowed with different tasks in mediating protection against influenza virus.
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