PU.1 and MYC transcriptional network defines synergistic drug responses to KIT and LSD1 inhibition in acute myeloid leukemia.
Brittany M CurtissJake VanCampenJommel MacaraegGarth L KongAkram TaherinasabMitsuhiro TsuchiyaWilliam M YasharYiu H TsangWesley HortonDaniel J ColemanJoseph EstabrookTheresa A LusardiGordon B MillsBrian J DrukerJulia E MaxsonTheodore P BraunPublished in: Leukemia (2022)
Responses to kinase-inhibitor therapy in AML are frequently short-lived due to the rapid development of resistance, limiting the clinical efficacy. Combination therapy may improve initial therapeutic responses by targeting pathways used by leukemia cells to escape monotherapy. Here we report that combined inhibition of KIT and lysine-specific demethylase 1 (LSD1) produces synergistic cell death in KIT-mutant AML cell lines and primary patient samples. This drug combination evicts both MYC and PU.1 from chromatin driving cell cycle exit. Using a live cell biosensor for AKT activity, we identify early adaptive changes in kinase signaling following KIT inhibition that are reversed with the addition of LSD1 inhibitor via modulation of the GSK3a/b axis. Multi-omic analyses, including scRNA-seq, ATAC-seq and CUT&Tag, confirm these mechanisms in primary KIT-mutant AML. Collectively, this work provides rational for a clinical trial to assess the efficacy of KIT and LSD1 inhibition in patients with KIT-mutant AML.
Keyphrases
- acute myeloid leukemia
- combination therapy
- cell cycle
- cell death
- clinical trial
- transcription factor
- cell proliferation
- genome wide
- allogeneic hematopoietic stem cell transplantation
- gene expression
- single cell
- rna seq
- dna damage
- dna methylation
- bone marrow
- gold nanoparticles
- cancer therapy
- randomized controlled trial
- case report
- study protocol
- stem cells
- acute lymphoblastic leukemia
- double blind
- smoking cessation
- sensitive detection
- electronic health record
- phase iii