Pluripotent hemopoietic stem cells are c-kit ^<low

Abstract: Pluripotent hemopoietic stem cells (P-HSCs) were thought to be c-kit ؉ , but recent reports indicate that they are c-kit low . In the present report, we provide evidence using Ly5 congenic mice that P-HSCs are c-kit

“…12,13,16 It is well documented that the c-kit/SCF system plays an important role in the early stage of hematopoiesis. 23,26,32,[37][38][39][40][41][42] Therefore, it is important to clarify the pattern of c-kit expression on primitive stem/progenitor cells, but there have been conflicting reports concerning this antigen on such cells. It was reported that LTC-IC and cell cycle dormant progenitors and blast cell colony-forming cells are enriched in the human BM-and CB-derived CD34 + c-kit low cell populations, respectively.…”

“…Katayama et al 40 proposed a model in which c-kit expression progresses from low levels on primitive progenitors to high levels on actively cycling progenitors. Very recently, Doi et al 41 clearly demonstrated that pluripotent hematopoietic stem cells with long-term repopulating activity are lin − /CD71 − /classI high /ckit Ͻlow cells but not lin − /CD71 − /c-kit low cells. They defined these cells, which appeared to be c-kit − on FACS analysis, as c-kit Ͻlow cells.…”

Human cord blood-derived primitive progenitors are enriched in CD34+c-kit− cells: correlation between long-term culture-initiating cells and telomerase expression

“…12,13,16 It is well documented that the c-kit/SCF system plays an important role in the early stage of hematopoiesis. 23,26,32,[37][38][39][40][41][42] Therefore, it is important to clarify the pattern of c-kit expression on primitive stem/progenitor cells, but there have been conflicting reports concerning this antigen on such cells. It was reported that LTC-IC and cell cycle dormant progenitors and blast cell colony-forming cells are enriched in the human BM-and CB-derived CD34 + c-kit low cell populations, respectively.…”

“…Katayama et al 40 proposed a model in which c-kit expression progresses from low levels on primitive progenitors to high levels on actively cycling progenitors. Very recently, Doi et al 41 clearly demonstrated that pluripotent hematopoietic stem cells with long-term repopulating activity are lin − /CD71 − /classI high /ckit Ͻlow cells but not lin − /CD71 − /c-kit low cells. They defined these cells, which appeared to be c-kit − on FACS analysis, as c-kit Ͻlow cells.…”

Human cord blood-derived primitive progenitors are enriched in CD34+c-kit− cells: correlation between long-term culture-initiating cells and telomerase expression

“…We prepared partially purified stem cell-enriched BMCs as previously described [26][27][28]. Briefly, 5-fluorouracil (Kyowa Hakko Kogyo; Tokyo, Japan) was injected into the peritoneal cavity of 4-week-old male Brown Norway rats (Clea Japan; Osaka, Japan) at 150 mg/kg body weight 48 hours before sacrifice.…”

Bone Marrow‐Derived Stem Cells Can Differentiate into Retinal Cells in Injured Rat Retina

“…Expression of FcR was considered because it has been observed on immature, antigencapturing DC (6). Cells also were stained for c-kit, a marker of early hemopoietic cells (20). Murine fetal liver-derived lin Ϫ ckit ϩ hemopoietic progenitor cells have been shown to develop into DC (21).…”

Identification of progenitor cells in long-term spleen stromal cultures that produce immature dendritic cells