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

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

Background Although 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 mut...

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Veröffentlicht in:Molecular cancer 2023-11, Vol.22 (1), p.1-177, Article 177
Hauptverfasser: Shin, Ji Eun, Kim, Soo-Hyun, Kong, Mingyu, Kim, Hwa-Ryeon, Yoon, Sungmin, Kee, Kyung-Mi, Kim, Jung Ah, Kim, Dong Hyeon, Park, So Yeon, Park, Jae Hyung, Kim, Hongtae, No, Kyoung Tai, Lee, Han-Woong, Gee, Heon Yung, Hong, Seunghee, Guan, Kun-Liang, Roe, Jae-Seok, Lee, Hyunbeom, Kim, Dong-Wook, Park, Hyun Woo
Format: Artikel
Sprache:eng
Schlagworte:
Acute myeloid leukemia
Animal models
Antibodies
Blast phase
CD36 antigen
Cell culture
Cell cycle
Cell death
Cell growth
Chemical compounds
Chronic myeloid leukemia
Development and progression
Drug resistance
Ethylenediaminetetraacetic acid
Explosions
Flow cytometry
FLT3
Flt3 protein
Health aspects
Hippo-YAP/TAZ pathway
Infections
Kinases
Leukemia
Localization
Malignancy
Medical prognosis
Medical research
Medicine, Experimental
Midostaurin
Molecular modelling
Nilotinib
Patients
Ponatinib
Product development
Prognosis
Protein-tyrosine kinase
Signal transduction
Stat3 protein
Therapeutic targets
Tyrosine
Viral infections
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Zusammenfassung:Background Although 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. Methods We 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.sup.+ CML patients. Results We reposition the significance of FLT3 in the acquisition of drug resistance in BP-CML, thereby, newly classify a FLT3.sup.+ 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.sup.+ BP-CML patients had significantly less favorable prognosis than FLT3.sup.- 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.sup.+ BCR::ABL1 cells and mouse xenograft models. Conclusion Here, 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. Graphical Keywords: FLT3, Drug resistance, Hippo-YAP/TAZ pathway, Blast phase, Ponatinib, Midostaurin, CML, AML, Cancer, CD36
ISSN:1476-4598
1476-4598
DOI:10.1186/s12943-023-01837-4