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. Author manuscript; available in PMC: 2015 Apr 24.
Published in final edited form as: Nature. 2014 Oct 5;514(7522):322–327. doi: 10.1038/nature13824

Extended Data Figure 9. Clonal analysis of haematopoiesis under transplantation conditions.

Extended Data Figure 9

a, Experimental flow chart showing viral infection of donor cells and longitudinal analysis of clonal dynamics in the transplant mouse. 2,000 DsRed+ LSK cells were transduced with retrovirus in the presence of TPO, Flt3 and SCF for 2 days and transferred to lethally irradiated recipients in the presence of 1×105 wild-type bone marrow cells. b, Distribution of PB Gr tags and their presence in B cells and T cells from recipient mouse AR1001 at three time points following transplantation. Tn tags unique to B cells or T cells are not shown. c, Single-cell analysis of PB granulocyte Tn tags from mouse AR1001 at 35 and 60 weeks after transplantation. d, A subset of dominant clones revealed in single-cell analysis (c) are stable in PB. e, Experimental flow chart showing purification and transplantation of LT-HSCs or LincKit+ BM cells from induced M2/HSB/Tn mice. 4 × 104 DsRed+ LT-HSCs or 5×104 DsRed+LincKit+ cells per recipient mouse were used. f–h and k–m, Distribution, recurrence, and lineage potential of PB Gr clones from recipient mouse AR856 receiving LT-HSC donor cells (f–h) and mouse AR541 receiving LincKit+ donor cells (k–m). Data are presented in the same manner as Fig. 2b–d. i, Single-cell analysis of granulocyte Tn tags from mouse AR856 25 weeks after transplantation. j, The dominant clone identified in single-cell (SC) analysis (clone no. 1 in i) is persistently detected in PB and BM from a single femur at 33 weeks. This clone is also detected in the LT-HSC compartment.