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Expression of myeloid Src-family kinases is associated with poor prognosis in AML and influences Flt3-ITD kinase inhibitor acquired resistance

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  • Ravi K Patel
  • Mark C Weir
  • Kexin Shen
  • Daniel Snyder
  • Vaughn S Cooper
  • Thomas E Smithgall

Abstract

Unregulated protein-tyrosine kinase signaling is a common feature of AML, often involving mutations in Flt3 and overexpression of myeloid Src-family kinases (Hck, Fgr, Lyn). Here we show that high-level expression of these Src kinases predicts poor survival in a large cohort of AML patients. To test the therapeutic benefit of Flt3 and Src-family kinase inhibition, we used the pyrrolopyrimidine kinase inhibitor A-419259. This compound potently inhibits Hck, Fgr, and Lyn as well as Flt3 bearing an activating internal tandem duplication (ITD). Flt3-ITD expression sensitized human TF-1 myeloid cells to growth arrest by A-419259, supporting direct action on the Flt3-ITD kinase domain. Cells transformed with the Flt3-ITD mutants D835Y and F691L were resistant to A-419259, while co-expression of Hck or Fgr restored inhibitor sensitivity to Flt3-ITD D835Y. Conversely, Hck and Fgr mutants with engineered A-419259 resistance mutations decreased sensitivity of TF-1/Flt3-ITD cells. To investigate de novo resistance mechanisms, A-419259-resistant Flt3-ITD+ AML cell populations were derived via long-term dose escalation. Whole exome sequencing identified a distinct Flt3-ITD kinase domain mutation (N676S/T) among all A-419259 target kinases in each of six independent resistant cell populations. These studies show that Hck and Fgr expression influences inhibitor sensitivity and the pathway to acquired resistance in Flt3-ITD+ AML.

Suggested Citation

  • Ravi K Patel & Mark C Weir & Kexin Shen & Daniel Snyder & Vaughn S Cooper & Thomas E Smithgall, 2019. "Expression of myeloid Src-family kinases is associated with poor prognosis in AML and influences Flt3-ITD kinase inhibitor acquired resistance," PLOS ONE, Public Library of Science, vol. 14(12), pages 1-29, December.
    • Handle: RePEc:plo:pone00:0225887
    DOI: 10.1371/journal.pone.0225887
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    1. Catherine C. Smith & Qi Wang & Chen-Shan Chin & Sara Salerno & Lauren E. Damon & Mark J. Levis & Alexander E. Perl & Kevin J. Travers & Susana Wang & Jeremy P. Hunt & Patrick P. Zarrinkar & Eric E. Sc, 2012. "Validation of ITD mutations in FLT3 as a therapeutic target in human acute myeloid leukaemia," Nature, Nature, vol. 485(7397), pages 260-263, May.
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