Figure 6
Figure 6. Apc haploinsufficiency affects the repopulating capacity of HSCs in vivo. (A) Mice with chimeric BM were generated by transplanting an equal number of wild-type CD45.1+CD45.2+ (CD45 heterozygous) BM cells and CD45.2+ (homozygous) BM cells from Mx1-Cre+Apcfl/+ or Mx1-Cre−Apcfl/+ mice 4 weeks after pI-pC induction of the Apc deletion. (B) Flow cytometric analysis of CD45.1- and CD45.2-stained PB cells from representative chimeric Mx1-Cre+Apcfl/+ or Mx1-Cre−Apcfl/+ mice 1 month after transplantation. The numbers indicate the percentage of cells in each population. (C) Histogram showing the relative ratio of CD45.2+ versus CD45.1+/CD45.2+-stained PB cells in Mx1-Cre−Apcfl/+ versus Mx1-Cre+Apcfl/+ chimeric mice examined at 1 to 4 months after transplantation (mean ± SD of 8-10 animals). *P < .05; **P < .01.

Apc haploinsufficiency affects the repopulating capacity of HSCs in vivo. (A) Mice with chimeric BM were generated by transplanting an equal number of wild-type CD45.1+CD45.2+ (CD45 heterozygous) BM cells and CD45.2+ (homozygous) BM cells from Mx1-Cre+Apcfl/+ or Mx1-CreApcfl/+ mice 4 weeks after pI-pC induction of the Apc deletion. (B) Flow cytometric analysis of CD45.1- and CD45.2-stained PB cells from representative chimeric Mx1-Cre+Apcfl/+ or Mx1-CreApcfl/+ mice 1 month after transplantation. The numbers indicate the percentage of cells in each population. (C) Histogram showing the relative ratio of CD45.2+ versus CD45.1+/CD45.2+-stained PB cells in Mx1-CreApcfl/+ versus Mx1-Cre+Apcfl/+ chimeric mice examined at 1 to 4 months after transplantation (mean ± SD of 8-10 animals). *P < .05; **P < .01.

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