High Density Domain-Focused CRISPR Screens Reveal Novel Epigenetic Regulators ofHOX/MEISActivation in Acute Myeloid Leukemia

Author:

Barbosa KarinaORCID,Deshpande Anagha,Perales Marlenne,Xiang Ping,Murad Rabi,Minkina AnnaORCID,Robertson Neil,Schischlik Fiorella,Lei Xue,Sun Younguk,Brown Adam,Amend Diana,Jeremias Irmela,Doench John G.,Humphries R. Keith,Ruppin Eytan,Shendure JayORCID,Mali Prashant,Adams Peter DORCID,Deshpande Aniruddha J.ORCID

Abstract

ABSTRACTAberrant expression of stem-cell-associated genes is a common feature in acute myeloid leukemia (AML) and is linked to leukemic self-renewal and therapy resistance. Using AF10-rearranged leukemia as a prototypical example displaying a recurrent “stemness” network activated in AML, we screened for chromatin regulators that sustain aberrant activation of these networks. We deployed a CRISPR-Cas9 screen with a bespoke domain-focused library and identified several novel chromatin-modifying complexes as regulators of the TALE domain transcription factor MEIS1, a key leukemia stem cell (LSC)-associated gene. CRISPR droplet sequencing revealed that many of these MEIS1 regulators coordinately controlled the transcription of several AML oncogenes. In particular, we identified a novel role for the Tudor-domain containing chromatin reader protein SGF29 in the transcription of key AML oncogenes. Furthermore, SGF29 deletion impaired leukemogenesis in models representative of multiple AML subtypes. Our studies reveal a novel role for SGF29 as a non-oncogenic dependency in AML and identify the SGF29 Tudor domain as an attractive target for drug discovery.

Publisher

Cold Spring Harbor Laboratory

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