Haematologica (Dec 2008)

The allele burden of JAK2 mutations remains stable over several years in patients with myeloproliferative disorders

  • Alexandre Theocharides,
  • Jakob R. Passweg,
  • Michael Medinger,
  • Renate Looser,
  • Sai Li,
  • Hui Hao-Shen,
  • Andreas S. Buser,
  • Alois Gratwohl,
  • André Tichelli,
  • Radek C. Skoda

DOI
https://doi.org/10.3324/haematol.13074
Journal volume & issue
Vol. 93, no. 12

Abstract

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In a retrospective single center study we determined the time course of the JAK2-V617F or JAK2 exon 12 allele burden in DNA from purified granulocytes from 48 patients with myeloproliferative disorders. The percentage of change between the first and last sample in JAK2-V617F positive patients without cytoreductive therapy (n=16) was only +9% during a follow-up of 36±13 months, reflecting a remarkably stable mutant allele burden. When treatment with hydroxyurea was initiated during the course of the study, we observed a significant decrease of the JAK2-V617F allele burden (n=6). However, in JAK2-V617F positive patients who were already on hydroxyurea treatment before the first blood sampling (n=14), we observed stable allelic ratios with a variance of only +3% during a follow-up of 34±16 months. Our data suggest that in untreated myeloproliferative disorders patients, from whom samples at diagnosis are not available, the JAK2 allele burden determined at later stages could be equally informative.