Disruption of the MYC Superenhancer Complex by Dual Targeting of FLT3 and LSD1 in Acute Myeloid Leukemia

William M. Yashar; Brittany M. Curtiss; Daniel J. Coleman; Jake VanCampen; Garth Kong; Jommel Macaraeg; Joseph Estabrook; Emek Demir; Nicola Long; Daniel Bottomly; Shannon K. McWeeney; Jeffrey W. Tyner; Brian J. Druker; Julia E. Maxson; Theodore P. Braun

doi:10.1158/1541-7786.MCR-22-0745

Disruption of the MYC Superenhancer Complex by Dual Targeting of FLT3 and LSD1 in Acute Myeloid Leukemia

William M. Yashar, Brittany M. Curtiss, Daniel J. Coleman, Jake VanCampen, Garth Kong, Jommel Macaraeg, Joseph Estabrook, Emek Demir, Nicola Long, Daniel Bottomly, Shannon K. McWeeney, Jeffrey W. Tyner, Brian J. Druker, Julia E. Maxson, Theodore P. Braun

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Abstract

Mutations in Fms-like tyrosine kinase 3 (FLT3) are common drivers in acute myeloid leukemia (AML) yet FLT3 inhibitors only provide modest clinical benefit. Prior work has shown that inhibitors of lysine-specific demethylase 1 (LSD1) enhance kinase inhibitor activity in AML. Here we show that combined LSD1 and FLT3 inhibition induces synergistic cell death in FLT3-mutant AML. Multi-omic profiling revealed that the drug combination disrupts STAT5, LSD1, and GFI1 binding at the MYC blood superenhancer, suppressing superenhancer accessibility as well as MYC expression and activity. The drug combination simultaneously results in the accumulation of repressive H3K9me1 methylation, an LSD1 substrate, at MYC target genes. We validated these findings in 72 primary AML samples with the nearly every sample demonstrating synergistic responses to the drug combination. Collectively, these studies reveal how epigenetic therapies augment the activity of kinase inhibitors in FLT3-ITD (internal tandem duplication) AML. Implications: This work establishes the synergistic efficacy of combined FLT3 and LSD1 inhibition in FLT3-ITD AML by disrupting STAT5 and GFI1 binding at the MYC blood-specific superenhancer complex. (Figure Presented).

Original language	English (US)
Pages (from-to)	631-647
Number of pages	17
Journal	Molecular Cancer Research
Volume	21
Issue number	7
DOIs	https://doi.org/10.1158/1541-7786.MCR-22-0745
State	Published - Jul 1 2023

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General Medicine

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Yashar, W. M., Curtiss, B. M., Coleman, D. J., VanCampen, J., Kong, G., Macaraeg, J., Estabrook, J., Demir, E., Long, N., Bottomly, D., McWeeney, S. K., Tyner, J. W., Druker, B. J., Maxson, J. E., & Braun, T. P. (2023). Disruption of the MYC Superenhancer Complex by Dual Targeting of FLT3 and LSD1 in Acute Myeloid Leukemia. Molecular Cancer Research, 21(7), 631-647. https://doi.org/10.1158/1541-7786.MCR-22-0745

Yashar, WM, Curtiss, BM, Coleman, DJ, VanCampen, J, Kong, G, Macaraeg, J, Estabrook, J, Demir, E, Long, N, Bottomly, D, McWeeney, SK , Tyner, JW , Druker, BJ , Maxson, JE & Braun, TP 2023, 'Disruption of the MYC Superenhancer Complex by Dual Targeting of FLT3 and LSD1 in Acute Myeloid Leukemia', Molecular Cancer Research, vol. 21, no. 7, pp. 631-647. https://doi.org/10.1158/1541-7786.MCR-22-0745

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title = "Disruption of the MYC Superenhancer Complex by Dual Targeting of FLT3 and LSD1 in Acute Myeloid Leukemia",

abstract = "Mutations in Fms-like tyrosine kinase 3 (FLT3) are common drivers in acute myeloid leukemia (AML) yet FLT3 inhibitors only provide modest clinical benefit. Prior work has shown that inhibitors of lysine-specific demethylase 1 (LSD1) enhance kinase inhibitor activity in AML. Here we show that combined LSD1 and FLT3 inhibition induces synergistic cell death in FLT3-mutant AML. Multi-omic profiling revealed that the drug combination disrupts STAT5, LSD1, and GFI1 binding at the MYC blood superenhancer, suppressing superenhancer accessibility as well as MYC expression and activity. The drug combination simultaneously results in the accumulation of repressive H3K9me1 methylation, an LSD1 substrate, at MYC target genes. We validated these findings in 72 primary AML samples with the nearly every sample demonstrating synergistic responses to the drug combination. Collectively, these studies reveal how epigenetic therapies augment the activity of kinase inhibitors in FLT3-ITD (internal tandem duplication) AML. Implications: This work establishes the synergistic efficacy of combined FLT3 and LSD1 inhibition in FLT3-ITD AML by disrupting STAT5 and GFI1 binding at the MYC blood-specific superenhancer complex. (Figure Presented).",

author = "Yashar, {William M.} and Curtiss, {Brittany M.} and Coleman, {Daniel J.} and Jake VanCampen and Garth Kong and Jommel Macaraeg and Joseph Estabrook and Emek Demir and Nicola Long and Daniel Bottomly and McWeeney, {Shannon K.} and Tyner, {Jeffrey W.} and Druker, {Brian J.} and Maxson, {Julia E.} and Braun, {Theodore P.}",

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doi = "10.1158/1541-7786.MCR-22-0745",

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AU - Yashar, William M.

AU - Curtiss, Brittany M.

AU - Coleman, Daniel J.

AU - VanCampen, Jake

AU - Kong, Garth

AU - Macaraeg, Jommel

AU - Estabrook, Joseph

AU - Demir, Emek

AU - Long, Nicola

AU - Bottomly, Daniel

AU - McWeeney, Shannon K.

AU - Tyner, Jeffrey W.

AU - Druker, Brian J.

AU - Maxson, Julia E.

AU - Braun, Theodore P.

PY - 2023/7/1

Y1 - 2023/7/1

N2 - Mutations in Fms-like tyrosine kinase 3 (FLT3) are common drivers in acute myeloid leukemia (AML) yet FLT3 inhibitors only provide modest clinical benefit. Prior work has shown that inhibitors of lysine-specific demethylase 1 (LSD1) enhance kinase inhibitor activity in AML. Here we show that combined LSD1 and FLT3 inhibition induces synergistic cell death in FLT3-mutant AML. Multi-omic profiling revealed that the drug combination disrupts STAT5, LSD1, and GFI1 binding at the MYC blood superenhancer, suppressing superenhancer accessibility as well as MYC expression and activity. The drug combination simultaneously results in the accumulation of repressive H3K9me1 methylation, an LSD1 substrate, at MYC target genes. We validated these findings in 72 primary AML samples with the nearly every sample demonstrating synergistic responses to the drug combination. Collectively, these studies reveal how epigenetic therapies augment the activity of kinase inhibitors in FLT3-ITD (internal tandem duplication) AML. Implications: This work establishes the synergistic efficacy of combined FLT3 and LSD1 inhibition in FLT3-ITD AML by disrupting STAT5 and GFI1 binding at the MYC blood-specific superenhancer complex. (Figure Presented).

AB - Mutations in Fms-like tyrosine kinase 3 (FLT3) are common drivers in acute myeloid leukemia (AML) yet FLT3 inhibitors only provide modest clinical benefit. Prior work has shown that inhibitors of lysine-specific demethylase 1 (LSD1) enhance kinase inhibitor activity in AML. Here we show that combined LSD1 and FLT3 inhibition induces synergistic cell death in FLT3-mutant AML. Multi-omic profiling revealed that the drug combination disrupts STAT5, LSD1, and GFI1 binding at the MYC blood superenhancer, suppressing superenhancer accessibility as well as MYC expression and activity. The drug combination simultaneously results in the accumulation of repressive H3K9me1 methylation, an LSD1 substrate, at MYC target genes. We validated these findings in 72 primary AML samples with the nearly every sample demonstrating synergistic responses to the drug combination. Collectively, these studies reveal how epigenetic therapies augment the activity of kinase inhibitors in FLT3-ITD (internal tandem duplication) AML. Implications: This work establishes the synergistic efficacy of combined FLT3 and LSD1 inhibition in FLT3-ITD AML by disrupting STAT5 and GFI1 binding at the MYC blood-specific superenhancer complex. (Figure Presented).

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Disruption of the MYC Superenhancer Complex by Dual Targeting of FLT3 and LSD1 in Acute Myeloid Leukemia

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