Synergistic effects on erythropoiesis, thrombopoiesis, and stem cell competitiveness in mice deficient in thrombopoietin and steel factor receptors
- 1 September 2004
- journal article
- Published by American Society of Hematology in Blood
- Vol. 104 (5) , 1306-1313
- https://doi.org/10.1182/blood-2004-04-1522
Abstract
The degree of redundancy between thrombopoietin (Tpo) and steel factor (SF) cytokine pathways in the regulation of hematopoiesis was investigated by generating mice lacking both c-Mpl and fully functional c-Kit receptors. Double-mutant c-Mpl–/–KitWv/Wv mice exhibited reduced viability, making up only 2% of the offspring from c-Mpl–/–KitWv/+ intercrosses. The thrombocytopenia and megakaryocytopenia characteristic of c-Mpl–/– mice was unchanged in c-Mpl–/–KitWv/Wv mice. However, the number of megakaryocytic colony forming units (CFU-Mks) was significantly reduced, particularly in the spleen. While KitWv/Wv mice, but not c-Mpl–/– mice, are anemic, the anemia was more severe in double-mutant c-Mpl–/–KitWv/Wv mice, indicating redundancy between Tpo and SF in erythropoiesis. At the primitive cell level, c-Mpl–/– and KitWv/Wv mice have similar phenotypes, including reduced progenitors, colony forming units–spleen (CFU-Ss), and repopulating activities. All of these parameters were exacerbated in double-mutant mice. c-Mpl–/–KitWv/Wv mice had 8-fold fewer clonogenic progenitor cells and at least 28-fold fewer CFU-Ss. c-Mpl–/– mice also demonstrated a reduced threshold requirement for nonmyeloablative transplant repopulation, a trait previously associated only with KitW mice, and the level of nonmyeloablative engraftment was significantly greater in c-Mpl–/–KitWv/Wv double mutants. Thus, c-Mpl–/–KitWv/Wv mice reveal nonredundant and synergistic effects of Tpo and SF on primitive hematopoietic cells.Keywords
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