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Genomic landscape and clonal evolution of acute myeloid leukemia with t(8;21): an international study on 331 patients

Authors :
Christen, Friederike
Hoyer, Kaja
Yoshida, Kenichi
Hou, Hsin-An
Waldhueter, Nils
Heuser, Michael
Hills, Robert K.
Chan, Willy
Hablesreiter, Raphael
Blau, Olga
Ochi, Yotaro
Klement, Piroska
Chou, Wen-Chien
Blau, Igor-Wolfgang
Tang, Jih-Luh
Zemojtel, Tomasz
Shiraishi, Yuichi
Shiozawa, Yusuke
Thol, Felicitas
Ganser, Arnold
Löwenberg, Bob
Linch, David C.
Bullinger, Lars
Valk, Peter J. M.
Tien, Hwei-Fang
Gale, Rosemary E.
Ogawa, Seishi
Damm, Frederik
Source :
Blood; March 2019, Vol. 133 Issue: 10 p1140-1151, 12p
Publication Year :
2019

Abstract

Acute myeloid leukemia with t(8;21)(q22;q22) is characterized by considerable clinical and biological heterogeneity leading to relapse in up to 40% of patients. We sequenced coding regions or hotspot areas of 66 recurrently mutated genes in a cohort of 331 t(8;21) patients. At least 1 mutation, in addition to t(8;21), was identified in 95%, with a mean of 2.2 driver mutations per patient. Recurrent mutations occurred in genes related to RAS/RTK signaling (63.4%), epigenetic regulators (45%), cohesin complex (13.6%), MYC signaling (10.3%), and the spliceosome (7.9%). Our study identified mutations in previously unappreciated genes: GIGYF2, DHX15, and G2E3. Based on high mutant levels, pairwise precedence, and stability at relapse, epigenetic regulator mutations were likely to occur before signaling mutations. In 34% of RAS/RTKmutated patients, we identified multiple mutations in the same pathway. Deep sequencing (~42?000×) of 126 mutations in 62 complete remission samples from 56 patients identified 16 persisting mutations in 12 patients, of whom 5 lacked RUNX1-RUNX1T1 in quantitative polymerase chain reaction analysis. KIThigh mutations defined by a mutant level =25% were associated with inferior relapse-free survival (hazard ratio, 1.96; 95% confidence interval, 1.22-3.15; P = .005). Together with age and white blood cell counts, JAK2, FLT3-internal tandem duplicationhigh, and KIThigh mutations were identified as significant prognostic factors for overall survival in multivariate analysis. Whole-exome sequencing was performed on 19 paired diagnosis, remission, and relapse trios. Exome-wide analysis showed an average of 16 mutations with signs of substantial clonal evolution. Based on the resemblance of diagnosis and relapse pairs, genetically stable (n = 13) and unstable (n = 6) subgroups could be identified.

Details

Language :
English
ISSN :
00064971 and 15280020
Volume :
133
Issue :
10
Database :
Supplemental Index
Journal :
Blood
Publication Type :
Periodical
Accession number :
ejs49696276
Full Text :
https://doi.org/10.1182/blood-2018-05-852822