TP-0903 is active in models of drug-resistant acute myeloid leukemia
Jae Yoon Jeon, … , Bhavana Bhatnagar, Sharyn D. Baker
Jae Yoon Jeon, … , Bhavana Bhatnagar, Sharyn D. Baker
Published December 3, 2020
Citation Information: JCI Insight. 2020;5(23):e140169. https://doi.org/10.1172/jci.insight.140169.
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Research Article Hematology Oncology

TP-0903 is active in models of drug-resistant acute myeloid leukemia

Abstract

Effective treatment for AML is challenging due to the presence of clonal heterogeneity and the evolution of polyclonal drug resistance. Here, we report that TP-0903 has potent activity against protein kinases related to STAT, AKT, and ERK signaling, as well as cell cycle regulators in biochemical and cellular assays. In vitro and in vivo, TP-0903 was active in multiple models of drug-resistant FLT3 mutant AML, including those involving the F691L gatekeeper mutation and bone marrow microenvironment–mediated factors. Furthermore, TP-0903 demonstrated preclinical activity in AML models with FLT3-ITD and common co-occurring mutations in IDH2 and NRAS genes. We also showed that TP-0903 had ex vivo activity in primary AML cells with recurrent mutations including MLL-PTD, ASXL1, SRSF2, and WT1, which are associated with poor prognosis or promote clinical resistance to AML-directed therapies. Our preclinical studies demonstrate that TP-0903 is a multikinase inhibitor with potent activity against multiple drug-resistant models of AML that will have an immediate clinical impact in a heterogeneous disease like AML.

Authors

Jae Yoon Jeon, Daelynn R. Buelow, Dominique A. Garrison, Mingshan Niu, Eric D. Eisenmann, Kevin M. Huang, Megan E. Zavorka Thomas, Robert H. Weber, Clifford J. Whatcott, Steve L. Warner, Shelley J. Orwick, Bridget Carmichael, Emily Stahl, Lindsey T. Brinton, Rosa Lapalombella, James S. Blachly, Erin Hertlein, John C. Byrd, Bhavana Bhatnagar, Sharyn D. Baker

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Figure 7

TP-0903 is active in AML with co-occurring FLT3-ITD and NRAS mutations.

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TP-0903 is active in AML with co-occurring FLT3-ITD and NRAS mutations. ...
(A) Sanger sequencing confirmation of the NRAS G12D mutation and RT-PCR showing increase NRAS expression after 24 hours of induction with 0.1 μg/mL doxycycline in MOLM13 cells with (+) and without (–) NRAS G12D. (B) Cell growth of MOLM13 and MOLM13 NRAS G12D when treated with DMSO or 15 nM of TP-0903 or gilteritinib induction with 0.1 μg/mL doxycycline (n = 6, representative of 3 independent experiments). (C and D) Inhibition of viability (CellTiterGlo, 72-hour treatment, n = 3) (C) or colony formation (14-day CFU assay, n = 2) (D) of human primary AML samples with FLT3-ITD and RAS pathway mutations treated with TKI indicated. P values were determined using unpaired 2-tailed Student’s t test and are indicated within the figure.