Title of article :
Imatinib effect on growth and signal transduction in polycythemia vera
Author/Authors :
Amos Gaikwad، نويسنده , , Srdan Verstovsek، نويسنده , , Donghoon Yoon، نويسنده , , KoTung Chang، نويسنده , , Taghi Manshouri، نويسنده , , Roberto Nussenzveig، نويسنده , , Jorge Cortés and Manuel de Le?n، نويسنده , , William Vainchenker، نويسنده , , Josef T. Prchal، نويسنده ,
Issue Information :
روزنامه با شماره پیاپی سال 2007
Pages :
8
From page :
931
To page :
938
Abstract :
Objective An activating mutation of Janus kinase 2 (JAK2) in majority of polycythemia vera (PV) and other myeloproliferative disorders was reported. As imatinib inhibits several tyrosine kinases, we studied its effect in PV. Patients and Methods We employed FDCP reporter cells expressing wild-type JAK2 and mutant JAK2V617F to study the efficacy of imatinib by cell proliferation assay and its effect on several cell-signaling events. Imatinibʹs efficacy was also examined on in vitro expanded native human erythroid progenitors. In addition, analysis of the percent JAK2 T-allele and phospho-signal transducer and activator of transcription-5 (STAT5) in granulocytes of PV patients following imatinib therapy was assessed. Results Imatinib showed a specific time- and dose-dependent growth inhibitory effect on FDCP cells expressing JAK2V617F, wherein we observed imatinibʹs inactivation of JAK2, STAT5 and cKIT proteins. In vitro expanded human PV erythroid progenitors were more sensitive to imatinib than normal erythroid progenitors and FDCP cells expressing JAK2V617F, with growth inhibition at concentrations attainable in vivo. In an ongoing clinical study, a PV patient showed strong correlation between the percent JAK2 T-allele and his responsiveness to imatinib therapy. Conclusion Our data elucidate the therapeutic benefit of imatinib seen in some PV patients. Our data suggest that JAK2/STAT5 and cKIT activation may be integrated. To our knowledge, this is the first report demonstrating imatinibʹs effect on PV erythroid progenitors. These studies underscore the limitation of experiments using cell lines expressing the gene of interest.
Journal title :
Experimental Hematology
Serial Year :
2007
Journal title :
Experimental Hematology
Record number :
514613
Link To Document :
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