Combinatorial Molecule Screening Identified a Novel Diterpene and the BET Inhibitor CPI-203 As Differentiation Inducers of Primary Acute Myeloid Leukemia Cells

Overview

Journal Haematologica

Specialty Hematology

Date 2020 Aug 29

PMID 32855276

Citations 4

Authors

Simon Hultmark

Aurelie Baudet

Ludwig Schmiderer

Pavan Prabhala

Sara Palma-Tortosa

Carl Sanden

Thoas Fioretos

Rajkumar Sasidharan

Christer Larsson

Soren Lehmann

Gunnar Juliusson

Fredrik Ek

Mattias Magnusson

Affiliations

Soon will be listed here.

Abstract

Combination treatment has proven effective for patients with acute promyelocytic leukemia, exemplifying the importance of therapy targeting multiple components of oncogenic regulation for a successful outcome. However, recent studies have shown that the mutational complexity of acute myeloid leukemia (AML) precludes the translation of molecular targeting into clinical success. Here, as a complement to genetic profiling, we used unbiased, combinatorial in vitro drug screening to identify pathways that drive AML and to develop personalized combinatorial treatments. First, we screened 513 natural compounds on primary AML cells and identified a novel diterpene (H4) that preferentially induced differentiation of FLT3 wild-type AML, while FLT3-ITD/mutations conferred resistance. The samples responding to H4, displayed increased expression of myeloid markers, a clear decrease in the nuclear-cytoplasmic ratio and the potential of re-activation of the monocytic transcriptional program reducing leukemia propagation in vivo. By combinatorial screening using H4 and molecules with defined targets, we demonstrated that H4 induces differentiation by the activation of the protein kinase C (PKC) signaling pathway, and in line with this, activates PKC phosphorylation and translocation of PKC to the cell membrane. Furthermore, the combinatorial screening identified a bromo- and extra-terminal domain (BET) inhibitor that could further improve H4-dependent leukemic differentiation in FLT3 wild-type monocytic AML. These findings illustrate the value of an unbiased, multiplex screening platform for developing combinatorial therapeutic approaches for AML.

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