C-Myc Inhibition Prevents Leukemia Initiation in Mice and Impairs the Growth of Relapsed and Induction Failure Pediatric T-ALL Cells

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2014 Jan 8

PMID 24394663

Citations 86

Authors

Justine E Roderick

Jessica Tesell

Leonard D Shultz

Michael A Brehm

Dale L Greiner

Marian H Harris

Lewis B Silverman

Stephen E Sallan

Alejandro Gutierrez

A Thomas Look

Jun Qi

James E Bradner

Michelle A Kelliher

Affiliations

Soon will be listed here.

Abstract

Although prognosis has improved for children with T-cell acute lymphoblastic leukemia (T-ALL), 20% to 30% of patients undergo induction failure (IF) or relapse. Leukemia-initiating cells (LICs) are hypothesized to be resistant to chemotherapy and to mediate relapse. We and others have shown that Notch1 directly regulates c-Myc, a known regulator of quiescence in stem and progenitor populations, leading us to examine whether c-Myc inhibition results in efficient targeting of T-ALL-initiating cells. We demonstrate that c-Myc suppression by small hairpin RNA or pharmacologic approaches prevents leukemia initiation in mice by eliminating LIC activity. Consistent with its anti-LIC activity in mice, treatment with the BET bromodomain BRD4 inhibitor JQ1 reduces C-MYC expression and inhibits the growth of relapsed and IF pediatric T-ALL samples in vitro. These findings demonstrate a critical role for c-Myc in LIC maintenance and provide evidence that MYC inhibition may be an effective therapy for relapsed/IF T-ALL patients.

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