Figure 4
Figure 4. Lethally irradiated WT mice reconstituted with CCR7−/− HSCs and MPCs (CCR7−/−→WT) show increased leukocyte influx into the lungs before and after A fumigatus challenge, compared with WT→WT chimeras. Fourteen days after HSCT, mice were left unchallenged or were injected with 2.0 × 106 conidia. Cellular infiltration into the lung was analyzed 48 hours after challenge. (A) Myeloid DCs were CD11c high, CD11b high, and MHC II+ cells. Neutrophils were CD11b high, Gr-1 high, and CD11c−. Monocytes/macrophages were CD11b+, F4/80+, and CD11c−. Plasmacytoid DCs were B220+ and CD11c+, CD4+ T cells were CD3+ and CD4+, and B cells were B220+ and CD11c−. (B) Dot plots of DCs and neutrophils demonstrate increased percentages of myeloid effector cells during IA (n = 4-5 mice per group. Data are representative of 3 separate experiments). *P < .05, when comparing WT or CCR7−/−→WT chimeric mice.

Lethally irradiated WT mice reconstituted with CCR7−/− HSCs and MPCs (CCR7−/−→WT) show increased leukocyte influx into the lungs before and after A fumigatus challenge, compared with WT→WT chimeras. Fourteen days after HSCT, mice were left unchallenged or were injected with 2.0 × 106 conidia. Cellular infiltration into the lung was analyzed 48 hours after challenge. (A) Myeloid DCs were CD11c high, CD11b high, and MHC II+ cells. Neutrophils were CD11b high, Gr-1 high, and CD11c. Monocytes/macrophages were CD11b+, F4/80+, and CD11c. Plasmacytoid DCs were B220+ and CD11c+, CD4+ T cells were CD3+ and CD4+, and B cells were B220+ and CD11c. (B) Dot plots of DCs and neutrophils demonstrate increased percentages of myeloid effector cells during IA (n = 4-5 mice per group. Data are representative of 3 separate experiments). *P < .05, when comparing WT or CCR7−/−→WT chimeric mice.

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