Figure 2
Figure 2. Serial transplantation demonstrates superior self-renewal of Lin−CD34+CD38−Rholo SRCs compared with Lin−CD34+CD38−Rhohi SRCs. Sorted cell populations were injected intrafemorally into preconditioned primary (1°) mice. After 7 to 10 weeks, the ability of SRCs to repopulate secondary (2°) mice was assessed separately for cells from the primary injected RF (A) and remaining BM (B). Secondary recipients were killed 7 to 10 weeks after transplantation, and human cell engraftment was assessed in the injected RF and remaining BM. Primary mice were injected with Lin−CD34+CD38−Rholo cells (•) or Lin−CD34+CD38−Rhohi cells (○). Bars indicate geometric means. (*) P < .05 versus Lin−CD34+CD38−Rhohi cells. (C) Southern blot analysis of repopulating clones in representative primary mice that received a transplant of Lin−CD34+CD38−Rholo cells and corresponding secondary recipients. Lanes were loaded with DNA obtained from RF or BM of a primary recipient and from the corresponding tissues of 2 secondary recipients injected with cells from the primary RF (*) or remaining BM (**). Self-renewing clones are indicated by arrowheads.

Serial transplantation demonstrates superior self-renewal of LinCD34+CD38Rholo SRCs compared with LinCD34+CD38Rhohi SRCs. Sorted cell populations were injected intrafemorally into preconditioned primary (1°) mice. After 7 to 10 weeks, the ability of SRCs to repopulate secondary (2°) mice was assessed separately for cells from the primary injected RF (A) and remaining BM (B). Secondary recipients were killed 7 to 10 weeks after transplantation, and human cell engraftment was assessed in the injected RF and remaining BM. Primary mice were injected with LinCD34+CD38Rholo cells (•) or LinCD34+CD38Rhohi cells (○). Bars indicate geometric means. (*) P < .05 versus LinCD34+CD38Rhohi cells. (C) Southern blot analysis of repopulating clones in representative primary mice that received a transplant of LinCD34+CD38Rholo cells and corresponding secondary recipients. Lanes were loaded with DNA obtained from RF or BM of a primary recipient and from the corresponding tissues of 2 secondary recipients injected with cells from the primary RF (*) or remaining BM (**). Self-renewing clones are indicated by arrowheads.

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