Prognostic impact of CEBPA mutational subgroups in adult AML

Author:

Georgi Julia-Annabell,Stasik SebastianORCID,Kramer Michael,Meggendorfer Manja,Röllig Christoph,Haferlach Torsten,Valk PeterORCID,Linch David,Herold TobiasORCID,Duployez NicolasORCID,Taube Franziska,Middeke Jan Moritz,Platzbecker UweORCID,Serve Hubert,Baldus Claudia D.ORCID,Muller-Tidow CarstenORCID,Haferlach ClaudiaORCID,Koch Sarah,Berdel Wolfgang E.,Woermann Bernhard J.ORCID,Krug Utz,Braess JanORCID,Hiddemann Wolfgang,Spiekermann KarstenORCID,Boertjes Emma L.,Hills Robert K.,Burnett Alan,Ehninger Gerhard,Metzeler KlausORCID,Rothenberg-Thurley Maja,Dufour Annika,Dombret Hervé,Pautas Cecile,Preudhomme Claude,Fenwarth LaureneORCID,Bornhäuser Martin,Gale RosemaryORCID,Thiede ChristianORCID

Abstract

AbstractDespite recent refinements in the diagnostic and prognostic assessment of CEBPA mutations in AML, several questions remain open, i.e. implications of different types of basic region leucin zipper (bZIP) mutations, the role of co-mutations and the allelic state. Using pooled primary data analysis on 1010 CEBPA-mutant adult AML patients, a comparison was performed taking into account the type of mutation (bZIP: either typical in-frame insertion/deletion (InDel) mutations (bZIPInDel), frameshift InDel or nonsense mutations inducing translational stop (bZIPSTOP) or single base-pair missense alterations (bZIPms), and transcription activation domain (TAD) mutations) and the allelic state (single (smCEBPA) vs. double mutant (dmCEBPA)). Only bZIPInDel patients had significantly higher rates of complete remission and longer relapse free and overall survival (OS) compared with all other CEBPA-mutant subgroups. Moreover, co-mutations in bZIPInDel patients (e.g. GATA2, FLT3, WT1 as well as ELN2022 adverse risk aberrations) had no independent impact on OS, whereas in non-bZIPInDel patients, grouping according to ELN2022 recommendations added significant prognostic information. In conclusion, these results demonstrate bZIPInDel mutations to be the major independent determinant of outcome in CEBPA-mutant AML, thereby refining current classifications according to WHO (including all dmCEBPA and smCEBPA bZIP) as well as ELN2022 and ICC recommendations (including CEBPA bZIPms).

Publisher

Springer Science and Business Media LLC

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