Targeting FLT3-TAZ signaling to suppress drug resistance in blast phase chronic myeloid leukemia

Ji Eun Shin; Soo-Hyun Kim; Mingyu Kong; Hwa-Ryeon Kim; Sungmin Yoon; Kyung-Mi Kee; Jung Ah Kim; Dong Hyeon Kim; So Yeon Park; Jae Hyung Park; Hongtae Kim; Kyoung Tai No; Han-Woong Lee; Heon Yung Gee; Seunghee Hong; Kun-Liang Guan; Jae-Seok Roe; Hyunbeom Lee; Dong-Wook Kim; Hyun Woo Park

doi:10.1186/s12943-023-01837-4

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Targeting FLT3-TAZ signaling to suppress drug resistance in blast phase chronic myeloid leukemia

Authors: Ji Eun Shin ; Soo-Hyun Kim ; Mingyu Kong ; Hwa-Ryeon Kim ; Sungmin Yoon ; Kyung-Mi Kee ; Jung Ah Kim ; Dong Hyeon Kim ; So Yeon Park ; Jae Hyung Park ; Hongtae Kim ; Kyoung Tai No ; Han-Woong Lee ; Heon Yung Gee ; Seunghee Hong ; Kun-Liang Guan ; Jae-Seok Roe ; Hyunbeom Lee ; Dong-Wook Kim ; Hyun Woo Park

Citation: MOLECULAR CANCER, Vol.22(1) : 177, 2023-11

Journal Title: MOLECULAR CANCER

Issue Date: 2023-11

MeSH: Animals ; Blast Crisis* / drug therapy ; Blast Crisis* / genetics ; Blast Crisis* / pathology ; Drug Resistance, Neoplasm / genetics ; Fusion Proteins, bcr-abl / genetics ; Humans ; Leukemia, Myelogenous, Chronic, BCR-ABL Positive* / genetics ; Mice ; Protein Kinase Inhibitors / pharmacology ; Signal Transduction ; fms-Like Tyrosine Kinase 3 / metabolism

Keywords: AML ; Blast phase ; CD36 ; CML ; Cancer ; Drug resistance ; FLT3 ; Hippo-YAP/TAZ pathway ; Midostaurin ; Ponatinib

Abstract: BackgroundAlthough the development of BCR::ABL1 tyrosine kinase inhibitors (TKIs) rendered chronic myeloid leukemia (CML) a manageable condition, acquisition of drug resistance during blast phase (BP) progression remains a critical challenge. Here, we reposition FLT3, one of the most frequently mutated drivers of acute myeloid leukemia (AML), as a prognostic marker and therapeutic target of BP-CML.MethodsWe generated FLT3 expressing BCR::ABL1 TKI-resistant CML cells and enrolled phase-specific CML patient cohort to obtain unpaired and paired serial specimens and verify the role of FLT3 signaling in BP-CML patients. We performed multi-omics approaches in animal and patient studies to demonstrate the clinical feasibility of FLT3 as a viable target of BP-CML by establishing the (1) molecular mechanisms of FLT3-driven drug resistance, (2) diagnostic methods of FLT3 protein expression and localization, (3) association between FLT3 signaling and CML prognosis, and (4) therapeutic strategies to tackle FLT3+ CML patients.ResultsWe reposition the significance of FLT3 in the acquisition of drug resistance in BP-CML, thereby, newly classify a FLT3+ BP-CML subgroup. Mechanistically, FLT3 expression in CML cells activated the FLT3-JAK-STAT3-TAZ-TEAD-CD36 signaling pathway, which conferred resistance to a wide range of BCR::ABL1 TKIs that was independent of recurrent BCR::ABL1 mutations. Notably, FLT3+ BP-CML patients had significantly less favorable prognosis than FLT3- patients. Remarkably, we demonstrate that repurposing FLT3 inhibitors combined with BCR::ABL1 targeted therapies or the single treatment with ponatinib alone can overcome drug resistance and promote BP-CML cell death in patient-derived FLT3+ BCR::ABL1 cells and mouse xenograft models.ConclusionHere, we reposition FLT3 as a critical determinant of CML progression via FLT3-JAK-STAT3-TAZ-TEAD-CD36 signaling pathway that promotes TKI resistance and predicts worse prognosis in BP-CML patients. Our findings open novel therapeutic opportunities that exploit the undescribed link between distinct types of malignancies.