Figure 2
Figure 2. CCR7−/− HSCs demonstrate enhanced myeloid reconstitution after HSCT. (A) Experimental scheme of a competitive reconstitution assay in which WT CD45.1 mice were lethally irradiated and reconstituted with 3.0 × 102 HSCs from WT CD45.1 and 3.0 × 102 HSCs from either WT (CD45.2) or CCR7−/− (CD45.2) mice, and 1.0 × 104 CMPs and GMPs from CD45.1 WT mice. Fourteen days after HSCT, flow cytometric analysis revealed a significant increase in the percentage and total number of spleen and lung cells derived from CCR7−/− HSCs, compared with WT HSCs. (B) Total number of cells and flow cytometric analysis of CD11bhi and Gr-1hi cells in the spleen 14 days after competitive transplantation. (C) Total number of cells and flow cytometric analysis of CD11bhi and Gr-1hi cells in the lung 14 days after competitive transplantation (n = 5 mice per group). *P < .05, when comparing cells originating from either WT or CCR7−/− HSCs.

CCR7−/− HSCs demonstrate enhanced myeloid reconstitution after HSCT. (A) Experimental scheme of a competitive reconstitution assay in which WT CD45.1 mice were lethally irradiated and reconstituted with 3.0 × 102 HSCs from WT CD45.1 and 3.0 × 102 HSCs from either WT (CD45.2) or CCR7−/− (CD45.2) mice, and 1.0 × 104 CMPs and GMPs from CD45.1 WT mice. Fourteen days after HSCT, flow cytometric analysis revealed a significant increase in the percentage and total number of spleen and lung cells derived from CCR7−/− HSCs, compared with WT HSCs. (B) Total number of cells and flow cytometric analysis of CD11bhi and Gr-1hi cells in the spleen 14 days after competitive transplantation. (C) Total number of cells and flow cytometric analysis of CD11bhi and Gr-1hi cells in the lung 14 days after competitive transplantation (n = 5 mice per group). *P < .05, when comparing cells originating from either WT or CCR7−/− HSCs.

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