BET inhibitors impair leukemic stem cell function only in defined oncogenic subgroups of acute myeloid leukaemias

Aline Massé,Louise Roulin,Justine Pasanisi,Justine Penneroux,Stéphanie Gachet,Marc Delord,Ashfaq Ali,Antônio José Alberdi,Jeannig Berrou,Marie Passet,Lucie Hernandez,Samuel Quentin,C. Gardin,Emmanuel Raffoux,Lionel Adès,Thorsten Braun,Jean Soulier,Emmanuelle Clappier,Hervé Dombret,Alexandre Puissant,Raphael Itzykson

BET inhibitors impair leukemic stem cell function only in defined oncogenic subgroups of acute myeloid leukaemias

2019

Abstract Bromodomain and Extra-Terminal inhibitors (BETi) such as OTX015 are active in Acute Myeloid Leukaemias (AML). Their activity on Leukemic Stem Cells (LSCs) is less documented. We interrogated the anti-LSC activity of OTX015 in a niche-like long-term culture in 26 primary AML samples and validated our findings in vivo. OTX015 impaired LSCs in AMLs harbouring Core Binding Factor or KMT2A gene fusions, NPM1 or chromatin/spliceosome genes mutations, but not in those with aneuploidy/TP53 mutations. In four patients, we dissected the transcriptomic footprint of Bet inhibition on LSCs versus blasts. Our results can instruct future clinical trials of BETi in AML.

Keywords:

Myeloid
Immunology
Aneuploidy
NPM1
Cancer research
Core binding factor
Chromatin
Biology
Stem cell
Spliceosome
Bromodomain

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