Genetics of acute myeloid leukemia in the elderly: mutation spectrum and clinical impact in intensively treated patients aged 75 years or older
Victoria V. Prassek,
Maja Rothenberg-Thurley,
Maria C. Sauerland,
Tobias Herold,
Hanna Janke,
Bianka Ksienzyk,
Nikola P. Konstandin,
Dennis Goerlich,
Utz Krug,
Andreas Faldum,
Wolfgang E. Berdel,
Bernhard Wörmann,
Jan Braess,
Stephanie Schneider,
Marion Subklewe,
Stefan K. Bohlander,
Wolfgang Hiddemann,
Karsten Spiekermann,
Klaus H. Metzeler
Affiliations
Victoria V. Prassek
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Maja Rothenberg-Thurley
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Maria C. Sauerland
Institute of Biostatistics and Clinical Research, University of Münster, Germany
Tobias Herold
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany;German Cancer Consortium (DKTK), Partner Site Munich, Germany;German Cancer Research Center (DKFZ), Heidelberg, Germany
Hanna Janke
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Bianka Ksienzyk
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Nikola P. Konstandin
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Dennis Goerlich
Institute of Biostatistics and Clinical Research, University of Münster, Germany
Utz Krug
Hospital Leverkusen, Germany
Andreas Faldum
Institute of Biostatistics and Clinical Research, University of Münster, Germany
Wolfgang E. Berdel
Institute of Biostatistics and Clinical Research, University of Münster, Germany
Bernhard Wörmann
Charité – University Hospital Berlin, Germany
Jan Braess
Department of Oncology and Hematology, Hospital Barmherzige Brüder, Regensburg, Germany
Stephanie Schneider
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Marion Subklewe
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany
Stefan K. Bohlander
Department of Molecular Medicine and Pathology, University of Auckland, New Zealand
Wolfgang Hiddemann
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany;German Cancer Consortium (DKTK), Partner Site Munich, Germany;German Cancer Research Center (DKFZ), Heidelberg, Germany
Karsten Spiekermann
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany;German Cancer Consortium (DKTK), Partner Site Munich, Germany;German Cancer Research Center (DKFZ), Heidelberg, Germany
Klaus H. Metzeler
Laboratory for Leukemia Diagnostics, Department of Medicine III, University Hospital, LMU Munich, Germany;German Cancer Consortium (DKTK), Partner Site Munich, Germany;German Cancer Research Center (DKFZ), Heidelberg, Germany
A cute myeloid leukemia is a disease of the elderly (median age at diagnosis, 65–70 years). The prognosis of older acute myeloid leukemia patients is generally poor. While genetic markers have become important tools for risk stratification and treatment selection in young and middle-aged patients, their applicability in very old patients is less clear. We sought to validate existing genetic risk classification systems and identify additional factors associated with outcomes in intensively treated patients aged ≥75 years. In 151 patients who received induction chemotherapy in the AMLCG-1999 trial, we investigated recurrently mutated genes using a targeted sequencing assay covering 64 genes. The median number of mutated genes per patient was four. The most commonly mutated genes were TET2 (42%), DNMT3A (35%), NPM1 (32%), SRSF2 (25%) and ASXL1 (21%). The complete remission rate was 44% and the 3-year survival was 21% for the entire cohort. While adverse-risk cytogenetics (MRC classification) were associated with shorter overall survival (P=0.001), NPM1 and FLT3-ITD mutations (present in 18%) did not have a significant impact on overall survival. Notably, none of the 13 IDH1-mutated patients (9%) reached complete remission. Consequently, the overall survival of this subgroup was significantly shorter than that of IDH1-wildtype patients (P
