Delta-1 enhances marrow and thymus repopulating ability of human CD34+CD38– cord blood cells
We investigated the effect of Notch signaling, a known regulator of cell fate in numerous developmental systems, on human hematopoietic precursors. We show that activation of endogenous Notch signaling in human CD34 + CD38 – cord blood precursors with immobilized Delta-1 in serum-free cultures conta...
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Veröffentlicht in: | The Journal of clinical investigation 2002-10, Vol.110 (8), p.1165-1174 |
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Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | We investigated the effect of Notch signaling, a known regulator of cell fate in numerous developmental systems, on human hematopoietic precursors. We show that activation of endogenous Notch signaling in human CD34
+
CD38
–
cord blood precursors with immobilized Delta-1 in serum-free cultures containing fibronectin and hematopoietic growth factors inhibited myeloid differentiation and induced a 100-fold increase in the number of CD34
+
cells compared with control cultures. Immobilized Delta-1 also induced a multifold expansion of cells with the phenotype of common lymphoid precursors (CD34
+
CD7
+
CD45RA
+
) and promoted the development of cytoplasmic CD3
+
T/NK cell precursors. IL-7 enhanced the promotion of T/NK cell differentiation by immobilized Delta-1, but granulocytic differentiation occurred when G-CSF was added. Transplantation into immunodeficient mice showed a substantial increase in myeloid and B cell engraftment in the marrow and also revealed thymic repopulation by CD3
+
T cells due to cells being cultured for a longer period with immobilized Delta-1. These data suggest that Delta-1 can enhance myeloid and lymphoid marrow-repopulating ability and promote the generation of thymus-repopulating T cell precursors. |
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ISSN: | 0021-9738 1558-8238 |
DOI: | 10.1172/JCI16167 |