TY - JOUR
T1 - Human primitive hematopoietic progenitor cells are more enriched in KIT(low) cells than in KIT(high) cells
AU - Gunji, Y.
AU - Nakamura, M.
AU - Osawa, H.
AU - Nagayoshi, K.
AU - Nakauchi, H.
AU - Miura, Y.
AU - Yanagisawa, M.
AU - Suda, T.
PY - 1993
Y1 - 1993
N2 - To clarify the phenotypes of various classes of human hematopoietic progenitor cells, we used a multicolor staining protocol in conjunction with CD34 and a newly developed mouse antihuman c-kit proto-oncogene product (KIT) monoclonal antibody (MoAb). We characterized three cell fractions in CD34+ cells that express KIT(low) and KIT(high) cells in addition to KIT- cells. A clonogenic assay showed that most granulocyte-macrophage colony-forming cells (GM-CFC) were present in CD34+ KIT(high) populations, whereas erythroid burst-forming cells (BFU-E) were detected mainly in the CD34+ KIT(low) population. CD34+-KIT- fraction contained a small number of BFU-E. Morphologic analysis showed that blast-like cells were more enriched in the CD34+KIT(low) fraction. KIT(low) cells contained CD34+CD38- cells that were considered to be very primitive progenitor cells, as determined by a replating assay. To clarify the biologic differences between both fractions, we examined the more primitive progenitor cell functions by assessing long- term culture-initiating cells (LTC-IC) on the stromal cells. At week 2, more CFC recovered from the culture in the fraction initiated with a CD34+KIT(high) population. However, more LTC-IC were present during weeks 5 to 9 in the CD34+KIT(low) population. These results indicate that primitive progenitors are more enriched in the KIT(low) population and that the KIT(high) population contains many GM-committed progenitor cells. We also showed that anti-KIT MoAb inhibited the ability of CD34+ cells to generate CFC on the stromal layer in the LTC system. This suppressive effect was more evident in the generation of BFU-E by CD34+KIT(low) cells. Moreover, we confirmed that CD34+KIT(high) cells emerged from CD34+KIT(low) cells during coculture with allogeneic stromal cells or from liquid culture in the presence of stem cell factor (SCF), interleukin-6, and erythropoietin. These results emphasize the pivotal role of the KIT and SCF interaction in hematopoiesis and indicate that KIT(low) cells are more primitive than KIT(high) cells.
AB - To clarify the phenotypes of various classes of human hematopoietic progenitor cells, we used a multicolor staining protocol in conjunction with CD34 and a newly developed mouse antihuman c-kit proto-oncogene product (KIT) monoclonal antibody (MoAb). We characterized three cell fractions in CD34+ cells that express KIT(low) and KIT(high) cells in addition to KIT- cells. A clonogenic assay showed that most granulocyte-macrophage colony-forming cells (GM-CFC) were present in CD34+ KIT(high) populations, whereas erythroid burst-forming cells (BFU-E) were detected mainly in the CD34+ KIT(low) population. CD34+-KIT- fraction contained a small number of BFU-E. Morphologic analysis showed that blast-like cells were more enriched in the CD34+KIT(low) fraction. KIT(low) cells contained CD34+CD38- cells that were considered to be very primitive progenitor cells, as determined by a replating assay. To clarify the biologic differences between both fractions, we examined the more primitive progenitor cell functions by assessing long- term culture-initiating cells (LTC-IC) on the stromal cells. At week 2, more CFC recovered from the culture in the fraction initiated with a CD34+KIT(high) population. However, more LTC-IC were present during weeks 5 to 9 in the CD34+KIT(low) population. These results indicate that primitive progenitors are more enriched in the KIT(low) population and that the KIT(high) population contains many GM-committed progenitor cells. We also showed that anti-KIT MoAb inhibited the ability of CD34+ cells to generate CFC on the stromal layer in the LTC system. This suppressive effect was more evident in the generation of BFU-E by CD34+KIT(low) cells. Moreover, we confirmed that CD34+KIT(high) cells emerged from CD34+KIT(low) cells during coculture with allogeneic stromal cells or from liquid culture in the presence of stem cell factor (SCF), interleukin-6, and erythropoietin. These results emphasize the pivotal role of the KIT and SCF interaction in hematopoiesis and indicate that KIT(low) cells are more primitive than KIT(high) cells.
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U2 - 10.1182/blood.v82.11.3283.3283
DO - 10.1182/blood.v82.11.3283.3283
M3 - Article
C2 - 7694677
AN - SCOPUS:0027517865
SN - 0006-4971
VL - 82
SP - 3283
EP - 3289
JO - Blood
JF - Blood
IS - 11
ER -