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HOXA9 forms a repressive complex with nuclear matrix-associated protein SAFB to maintain acute myeloid leukemia

相互作用体 髓系白血病 生物 染色质 细胞生物学 癌症研究 染色质重塑 遗传学 基因
作者
Shuchi Agrawal‐Singh,Jaana Bagri,George Giotopoulos,Dhoyazan Azazi,Shubha Anand,Anne-Sophie Bach,Frances Stedham,Sarah J. Horton,Robin Antrobus,Jack W. Houghton,George S. Vassiliou,Daniel Sasca,Haiyang Yun,Anthony D. Whetton,Brian J.P. Huntly
出处
期刊: [Cold Spring Harbor Laboratory]
被引量:1
标识
DOI:10.1101/2022.10.12.511919
摘要

Abstract HOXA9 is commonly upregulated in acute myeloid leukemia (AML), where it confers poor prognosis. Characterising the protein interactome of endogenous HOXA9 in human AML, we identified a chromatin complex of HOXA9 with the nuclear matrix attachment protein-SAFB. SAFB perturbation phenocopied HOXA9 knockout to decrease AML proliferation, increase differentiation and apoptosis in vitro and prolonged survival in vivo . Integrated genomic, transcriptomic and proteomic analyses further demonstrated that the HOXA9-SAFB-chromatin complex associates with NuRD and HP1γ to repress the expression of factors associated with differentiation and apoptosis, including NOTCH, CEBP δ, S100A8 , and CDKN1A . Chemical or genetic perturbation of NuRD and HP1γ catalytic activity also triggered differentiation, apoptosis and the induction of these tumor-suppressive genes. Importantly, this mechanism is operative in other HOXA9-dependent AML genotypes. This mechanistic insight demonstrates active HOXA9 -dependent differentiation block as a potent mechanism of disease maintenance in AML, that may be amenable to therapeutic intervention via therapies targeting the HOXA9/SAFB interface and/or NuRD and HP1γ activity. Key Points - Identification of the endogenous human HOXA9 protein interactome in AML - HOXA9 forms a repressive complex with S/MAR binding protein (SAFB) that is critical for the maintenance of AML by facilitating proliferation and preventing differentiation and cell death. - The HOXA9/SAFB (H9SB) complex represses gene expression via recruitment of NuRD and HP1γ.

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