Haematologica (Mar 2013)

Ruxolitinib as potential targeted therapy for patients with JAK2 rearrangements

  • Andrew Chase,
  • Catherine Bryant,
  • Joannah Score,
  • Claudia Haferlach,
  • Vera Grossmann,
  • Juliana Schwaab,
  • Wolf-Karsten Hofmann,
  • Andreas Reiter,
  • Nicholas C.P. Cross

DOI
https://doi.org/10.3324/haematol.2012.067959
Journal volume & issue
Vol. 98, no. 3

Abstract

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JAK2 fusion genes are rare but recurrent abnormalities associated with diverse, clinically heterogeneous hematologic malignancies. Here we assess the JAK1/2 inhibitor ruxolitinib as therapy for patients with JAK2-rearrangement associated myeloproliferative neoplasms (MPN). Ruxolitinib-treated Ba/F3 cells transformed to IL3 independence by ETV6-JAK2 showed reduced proliferation and survival (IC50 = 370 nM) compared with KG1A or Ba/F3 cells transformed by BCR-ABL1, SPBN1-FLT3 and ZMYM2-FGFR1 (IC50 > 10 μM for all). Inhibition was associated with reduced phosphorylation of ETV6-JAK2, ERK, STAT5 and AKT. Primary cell growth from 2 patients with JAK2 rearrangement and one patient with JAK2 amplification was assessed in methylcellulose assays. Reduced colony growth was seen for all patients in ruxolitinib-treated cultures compared with healthy controls (n=7). Fluorescence in situ hybridization showed reduced growth of JAK2-rearrangement positive colonies compared to JAK2-rearrangement negative colonies. Our data, therefore, provide evidence that ruxolitinib is a promising therapy for treatment of patients with JAK2 fusion genes.