Mutant CEBPA directly drives the expression of the targetable tumor-promoting factor CD73 in AML.
Janus Schou JakobsenLinea G LaursenMikkel Bruhn SchusterSachin PundhirErwin M SchoofYing GeTeresa d'AltriKristoffer Vitting-SeerupNicolas RapinColine GentilJohan JendholmKim Theilgaard-MönchKristian ReckzehLars BullingerKonstanze DöhnerPeter HoklandJude FitzgibbonBo Torben PorsePublished in: Science advances (2019)
The key myeloid transcription factor (TF), CEBPA, is frequently mutated in acute myeloid leukemia (AML), but the direct molecular effects of this leukemic driver mutation remain elusive. To investigate CEBPA mutant AML, we performed microscale, in vivo chromatin immunoprecipitation sequencing and identified a set of aberrantly activated enhancers, exclusively occupied by the leukemia-associated CEBPA-p30 isoform. Comparing gene expression changes in human CEBPA mutant AML and the corresponding Cebpa Lp30 mouse model, we identified Nt5e, encoding CD73, as a cross-species AML gene with an upstream leukemic enhancer physically and functionally linked to the gene. Increased expression of CD73, mediated by the CEBPA-p30 isoform, sustained leukemic growth via the CD73/A2AR axis. Notably, targeting of this pathway enhanced survival of AML-transplanted mice. Our data thus indicate a first-in-class link between a cancer driver mutation in a TF and a druggable, direct transcriptional target.
Keyphrases
- acute myeloid leukemia
- transcription factor
- gene expression
- allogeneic hematopoietic stem cell transplantation
- wild type
- poor prognosis
- mouse model
- genome wide
- binding protein
- endothelial cells
- copy number
- single cell
- papillary thyroid
- squamous cell carcinoma
- electronic health record
- adipose tissue
- skeletal muscle
- machine learning
- insulin resistance
- big data
- cancer therapy
- dna binding
- drug delivery
- squamous cell
- dendritic cells
- induced pluripotent stem cells