Project 4: BCR-ABL unabhängige Genmutatonen
Prevalence and dynamics of BCR-ABL independent gene mutations in chronic phase CML patients
Lioba Ruppert1, Jenny Rinke1, Anja Waldau1, Andreas Hochhaus1, Thomas Ernst1
- Abteilung Hämatologie/Onkologie, Klinik für Innere Medizin II, Universitätsklinikum Jena
Introduction: Living without treatment has become a realistic aim for patients with chronic myeloid leukemia (CML) who achieved durable deep molecular remission under treatment with tyrosine kinase inhibitors (TKI). Recently, we have identified novel BCR-ABL independent gene mutations in newly diagnosed CML patients whereby mutations in epigenetic modifier genes were most common. However, prevalence, kinetics and prognostic significance of such mutations in a clinically well-characterized patient population need to be investigated systematically.
Methods: A total of 100 chronic phase CML patients from the German CML-V (TIGER) trial were investigated by targeted deep next-generation sequencing (NGS) covering 54 genes frequently mutated in myeloid malignancies. Paired samples at diagnosis and after 12 months of therapy were investigated to study mutation dynamics. If available, follow-up samples after 24 month (87/100 patients) and 36 months (39/100 patients) of therapy were also investigated.
Results: Thirty-five different mutations were detected in 32/100 patients (32%) affecting the genes ASXL1, BCOR, CALR, CUX1, DNMT3A, FBXW7, GATA2, IKZF1, JAK2, NOTCH1, RUNX1, STAG2, TET2, TP53, U2AF1 and WT1. ASXL1 (n=11) and DNMT3A (n=4) were the most common mutations. In five patients more than one mutation was identified. 26/100 patients (26%) showed at least one mutation at diagnosis. Analysis of follow-up samples revealed that in 20 patients the mutations disappeared during TKI treatment. In 6 patients the mutation persisted indicating that the mutation preceded the BCR-ABL translocation. In 2/87 patients (2%) the initial mutation re-emerged at month 24 after disappearance at month 12. In 8/100 patients (8%) a new mutation occurred at month 12; four of these mutations vanished and 8 persisted in further follow-up samples. So far, only one patient showed a mutation first to emerge at month 24.
Conclusions: BCR-ABL independent gene mutations were frequently identified in chronic phase CML patients at diagnosis. In a minority of patients such mutations seem to precede the BCR-ABL translocation indicating a multistep pathogenesis in CML. BCR-ABL independent gene mutations were found to vary in their dynamics during TKI treatment and may function as important cofactors in the evolution and persistence of the disease.