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Publication : Activated Fps/Fes tyrosine kinase regulates erythroid differentiation and survival.

First Author  Sangrar W Year  2004
Journal  Exp Hematol Volume  32
Issue  10 Pages  935-45
PubMed ID  15504549 Mgi Jnum  J:93227
Mgi Id  MGI:3056254 Doi  10.1016/j.exphem.2004.07.004
Citation  Sangrar W, et al. (2004) Activated Fps/Fes tyrosine kinase regulates erythroid differentiation and survival. Exp Hematol 32(10):935-45
abstractText  OBJECTIVE: A substantial body of evidence implicates the cytoplasmic protein tyrosine kinase Fps/Fes in regulation of myeloid differentiation and survival. In this study we wished to determine if Fps/Fes also plays a role in the regulation of erythropoiesis. METHODS: Mice tissue-specifically expressing a 'gain-of-function' mutant fps/fes transgene (fps(MF)) encoding an activated variant of Fps/Fes (MFps), were used to explore the in vivo biological role of Fps/Fes. Erythropoiesis in these mice was assessed by hematological analysis, lineage marker analysis, bone-marrow colony assays, and biochemical approaches. RESULTS: fps(MF) mice displayed reductions in peripheral red cell counts. However, there was an accumulation of immature erythroid precursors, which displayed increased survival. Fps/Fes and the related Fer kinase were both detected in early erythroid progenitors/blasts and in mature red cells. Fps/Fes was also activated in response to erythropoietin (EPO) and stem cell factor (SCF), two critical factors in erythroid development. In addition, increased Stat5A/B activation and reduced Erk1/2 phosphorylation was observed in fps(MF) primary erythroid cells in response to EPO or SCF, respectively. CONCLUSIONS: These data support a role for Fps/Fes in regulating the survival and differentiation of erythroid cells through modulation of Stat5A/B and Erk kinase pathways induced by EPO and SCF. The increased numbers and survival of erythroid progenitors from fps(MF) mice, and their differential responsiveness to SCF and EPO, implicates Fps/Fes in the commitment of multilineage progenitors to the erythroid lineage. The anemic phenotype in fps(MF) mice suggests that downregulation of Fps/Fes activity might be required for terminal erythroid differentiation.
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