MLL-AF9– and HOXA9-mediated acute myeloid leukemia stem cell self-renewal requires JMJD1C
Nan Zhu, … , Robert G. Roeder, Scott A. Armstrong
Nan Zhu, … , Robert G. Roeder, Scott A. Armstrong
Published February 15, 2016
Citation Information: J Clin Invest. 2016;126(3):997-1011. https://doi.org/10.1172/JCI82978.
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MLL-AF9– and HOXA9-mediated acute myeloid leukemia stem cell self-renewal requires JMJD1C

Abstract

Self-renewal is a hallmark of both hematopoietic stem cells (HSCs) and leukemia stem cells (LSCs); therefore, the identification of mechanisms that are required for LSC, but not HSC, function could provide therapeutic opportunities that are more effective and less toxic than current treatments. Here, we employed an in vivo shRNA screen and identified jumonji domain–containing protein JMJD1C as an important driver of MLL-AF9 leukemia. Using a conditional mouse model, we showed that loss of JMJD1C substantially decreased LSC frequency and caused differentiation of MLL-AF9– and homeobox A9–driven (HOXA9-driven) leukemias. We determined that JMJD1C directly interacts with HOXA9 and modulates a HOXA9-controlled gene-expression program. In contrast, loss of JMJD1C led to only minor defects in blood homeostasis and modest effects on HSC self-renewal. Together, these data establish JMJD1C as an important mediator of MLL-AF9– and HOXA9-driven LSC function that is largely dispensable for HSC function.

Authors

Nan Zhu, Mo Chen, Rowena Eng, Joshua DeJong, Amit U. Sinha, Noushin F. Rahnamay, Richard Koche, Fatima Al-Shahrour, Janna C. Minehart, Chun-Wei Chen, Aniruddha J. Deshpande, Haiming Xu, S. Haihua Chu, Benjamin L. Ebert, Robert G. Roeder, Scott A. Armstrong

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Figure 3

JMJD1C interacts with HOXA9 and modulates a HOXA9-controlled gene-expression program.

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JMJD1C interacts with HOXA9 and modulates a HOXA9-controlled gene-expres...
(A) Heat map of differentially expressed genes in MLL-AF9 leukemia cells 6 days after loss of JMJD1C. (B) GSEA analysis result showing enrichment of HOXA9 repressed genes (37) and HOXA9 bound and repressed genes (44). NES, normalized enrichment score. (C) Co-IP of HA-HOXA9 and KDM3A family members in 293T cells transfected with indicated plasmids. (D) GST-binding assay using bacteria expressed and purified GST-HOXA9 and baculovirus system expressed and purified flag-JMJD1C. See also Supplemental Figure 3 and Supplemental Table 4.