Figure 5
Figure 5. Bone marrow cells from Gata1low mice engraft preferentially the extramedullary sites of the recipients. (A) Hematoxylin-eosin and CD45 immunostaining of liver sections from an untreated NOD/SCID female and from a NOD/SCID female that received a transplant of bone marrow cells from a Gata1low/0 male. The presence of cells with the Gata1+ (220 bp, 2 alleles per cell) and Gata1low (370 bp, one allele per cell) genotype in blood, bone marrow, spleen, and liver of representative NOD/SCID mice that received a transplant from either wild-type (C1-1) or Gata1low (2 mice, TIP87 and TIP 66) mice is presented on the bottom. Results are representative of those obtained in 12 animals that underwent transplantation. Magnification ×20 in the panels and ×40 in the insets. (B) Frequency of cells expressing a lymphocyte (B220pos or CD4pos), granulomonocyte (Mac3pos or Gr1pos), and MK (CD41pos/CD61pos) phenotype in the blood and of those expressing a stem cell (Sca1pos/CD117pos), erythroid (CD71pos/TER119pos), and MK (CD41pos/CD61pos) phenotype in the marrow, spleen, and liver of a representative NOD/SCID mouse that received a transplant 2 months earlier of 106 Gata1low bone marrow cells. Similar results were observed in 6 additional mice that underwent transplantation. The presence of cells with the Gata1+ (220 bp) and Gata1low (370 bp) genotype among the individual populations purified by sorting (> 90% pure by reanalysis) was assessed by PCR and presented on the right. Representative PCR analyses of cells purified from 3 representative recipients (each line is an individual mouse; A, B, or C). Representative isotype controls for the FACS analyses are presented in supplemental Figure 3.

Bone marrow cells from Gata1low mice engraft preferentially the extramedullary sites of the recipients. (A) Hematoxylin-eosin and CD45 immunostaining of liver sections from an untreated NOD/SCID female and from a NOD/SCID female that received a transplant of bone marrow cells from a Gata1low/0 male. The presence of cells with the Gata1+ (220 bp, 2 alleles per cell) and Gata1low (370 bp, one allele per cell) genotype in blood, bone marrow, spleen, and liver of representative NOD/SCID mice that received a transplant from either wild-type (C1-1) or Gata1low (2 mice, TIP87 and TIP 66) mice is presented on the bottom. Results are representative of those obtained in 12 animals that underwent transplantation. Magnification ×20 in the panels and ×40 in the insets. (B) Frequency of cells expressing a lymphocyte (B220pos or CD4pos), granulomonocyte (Mac3pos or Gr1pos), and MK (CD41pos/CD61pos) phenotype in the blood and of those expressing a stem cell (Sca1pos/CD117pos), erythroid (CD71pos/TER119pos), and MK (CD41pos/CD61pos) phenotype in the marrow, spleen, and liver of a representative NOD/SCID mouse that received a transplant 2 months earlier of 106 Gata1low bone marrow cells. Similar results were observed in 6 additional mice that underwent transplantation. The presence of cells with the Gata1+ (220 bp) and Gata1low (370 bp) genotype among the individual populations purified by sorting (> 90% pure by reanalysis) was assessed by PCR and presented on the right. Representative PCR analyses of cells purified from 3 representative recipients (each line is an individual mouse; A, B, or C). Representative isotype controls for the FACS analyses are presented in supplemental Figure 3.

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