Recently, the ligand for c-mpl, a member of the family of cytokine receptors, was cloned and found to be a physiologic regulator of platelet homeostasis. We report that megakaryocyte growth and development factor (MGDF, thrombopoietin [TPO], c-mpl ligand ) induces differentiation in a majority of mpl-transfected 32D cells, while interleukin (IL)-3 is exclusively mitogenic in this system. MGDF differentiation, as measured by decreased proliferation, changes in cellular morphology, increased adherence, and downregulation of very late antigen (VLA)-4, is dominant over IL-3 proliferation. MGDF induces tyrosine-phosphorylation of mpl, JAK2, SHC, SHPTP-1 (HCP, motheaten) and SHPTP-2 (Syp, PTP-1D) within 30 seconds of stimulation, as well as of vav and MAPK with slightly delayed kinetics. A fraction of mpl and JAK2 is preassociated, and the stoichiometry of this complex is unaltered by cytokine stimulation. After MGDF stimulation, we detect interactions among SHC, grb2, SHPTP-1, SHPTP-2, and the mpl/JAK2 complex. IL-3 induces phosphorylation of the above proteins with the exception of mpl and also causes weak JAK1 phosphorylation. Although similar in composition, the MGDF- and IL-3-induced complexes of signal transducers appear to be assembled in different configurations, especially with respect to SHPTP-2. Both MGDF and IL-3 induce tyrosine phosphorylation of STAT3 (APRF) and STAT5 (MGF), with MGDF favoring STAT3 while IL-3 predominantly causes STAT5 phosphorylation. In addition, some proteins become tyrosine-phosphorylated in response to MGDF only, suggesting that we may have detected differentiation- specific signal transducers. These include a number of high-molecular- weight proteins (140 to 200 kD) and one 28-kD protein that becomes tyrosine-phosphorylated only briefly.
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December 15, 1995
Megakaryocyte growth and development factor and interleukin-3 induce patterns of protein-tyrosine phosphorylation that correlate with dominant differentiation over proliferation of mpl-transfected 32D cells
SX Mu,
SX Mu
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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M Xia,
M Xia
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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G Elliott,
G Elliott
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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J Bogenberger,
J Bogenberger
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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S Swift,
S Swift
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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L Bennett,
L Bennett
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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DL Lappinga,
DL Lappinga
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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R Hecht,
R Hecht
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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R Lee,
R Lee
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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CJ Saris
CJ Saris
Department of Developmental Biology, Amgen Inc, Thousand Oaks, CA 91320, USA.
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Blood (1995) 86 (12): 4532–4543.
Citation
SX Mu, M Xia, G Elliott, J Bogenberger, S Swift, L Bennett, DL Lappinga, R Hecht, R Lee, CJ Saris; Megakaryocyte growth and development factor and interleukin-3 induce patterns of protein-tyrosine phosphorylation that correlate with dominant differentiation over proliferation of mpl-transfected 32D cells. Blood 1995; 86 (12): 4532–4543. doi: https://doi.org/10.1182/blood.V86.12.4532.bloodjournal86124532
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December 15 1995
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