BMC Cancer (Jul 2008)

<it>EVI1 </it>activation in blast crisis CML due to juxtaposition to the rare 17q22 partner region as part of a 4-way variant translocation t(9;22)

  • Verhasselt Bruno,
  • Dierick Jan,
  • Carlier Andre,
  • Cauwelier Barbara,
  • Poppe Bruce,
  • De Weer An,
  • Philippé Jan,
  • Van Roy Nadine,
  • Speleman Frank

DOI
https://doi.org/10.1186/1471-2407-8-193
Journal volume & issue
Vol. 8, no. 1
p. 193

Abstract

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Abstract Background Variant translocations t(9;22) occur in 5 to 10% of newly diagnosed CMLs and additional genetic changes are present in 60–80% of patients in blast crisis (BC). Here, we report on a CML patient in blast crisis presenting with a four-way variant t(9;22) rearrangement involving the EVI1 locus. Methods Dual-colour Fluorescence In Situ Hybridisation was performed to unravel the different cytogenetic aberrations. Expression levels of EVI1 and BCR/ABL1 were investigated using real-time quantitative RT-PCR. Results In this paper we identified a patient with a complex 4-way t(3;9;17;22) which, in addition to BCR/ABL1 gene fusion, also resulted in EVI1 rearrangement and overexpression. Conclusion This report illustrates how a variant t(9;22) translocation can specifically target a second oncogene most likely contributing to the more aggressive phenotype of the disease. Molecular analysis of such variants is thus warranted to understand the phenotypic consequences and to open the way for combined molecular therapies in order to tackle the secondary oncogenic effect which is unresponsive to imatinib treatment.