Defining the Transcriptional Control of Pediatric AML Highlights RARA As a Superenhancer-regulated Druggable Dependency

Overview

Journal Blood Adv

Specialty Hematology

Date 2021 Sep 20

PMID 34543389

Citations 5

Authors

Monika W Perez

Oscar Sias-Garcia

Alfred Daramola

Helen Wei

Maci Terrell

Raushan Rashid

Woojun D Park

Kevin Duong

Terzah M Horton

Feng Li

Nikitha Cherayil

Jost Vrabic Koren

Vincent U Gant

Jacob J Junco

Choladda V Curry

Alexandra M Stevens

Charles Y Lin

Joanna S Yi

Affiliations

Soon will be listed here.

Abstract

Somatic mutations are rare in pediatric acute myeloid leukemia (pAML), indicating that alternate strategies are needed to identify targetable dependencies. We performed the first enhancer mapping of pAML in 22 patient samples. Generally, pAML samples were distinct from adult AML samples, and MLL (KMT2A)-rearranged samples were also distinct from non-KMT2A-rearranged samples. Focusing specifically on superenhancers (SEs), we identified SEs associated with many known leukemia regulators. The retinoic acid receptor alpha (RARA) gene was differentially regulated in our cohort, and a RARA-associated SE was detected in 64% of the study cohort across all cytogenetic and molecular subtypes tested. RARA SE+ pAML cell lines and samples exhibited high RARA messenger RNA levels. These samples were specifically sensitive to the synthetic RARA agonist tamibarotene in vitro, with slowed proliferation, apoptosis induction, differentiation, and upregulated retinoid target gene expression, compared with RARA SE- samples. Tamibarotene prolonged survival and suppressed the leukemia burden of an RARA SE+ pAML patient-derived xenograft mouse model compared with a RARA SE- patient-derived xenograft. Our work shows that examining chromatin regulation can identify new, druggable dependencies in pAML and provides a rationale for a pediatric tamibarotene trial in children with RARA-high AML.

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