Supraphysiologic levels of the AML1-ETO isoform AE9a are essential for transformation

Link, Kevin A.; Lin, Shuo; Shrestha, Mahesh; Bowman, Melissa; Wunderlich, Mark; Bloomfield, Clara D.; Huang, Gang; Mulloy, James C.

doi:10.1073/pnas.1524225113

Cited by 14 publications

(18 citation statements)

References 47 publications

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“…MSCV-IRES-GFP/THY.1 (MIG/MIT) and MSCV-AE-IRES-GFP/THY.1 retroviral vectors were as described. 10,20 pSIN-TREtight-DsRED-IRES and MSCV-GFP-IRES-tTA retroviral vectors were generously provided by Johannes Zuber. Insertion of AE was subcloned into pSIN-TREtight-DsRED-IRES to build an AE-tet-off system.…”

Section: Plasmids and Reagentsmentioning

confidence: 99%

“…We and others have shown that expression of AE in human CD34 1 hematopoietic stem and progenitor cells (HSPCs) causes dysregulated differentiation and increased self-renewal of cells but without inducing AML, 9,10 serving as an ideal model to study the preleukemic stage of t(8;21) AML (AE cells). Until now, the mechanism by which AE programs progenitor cells into preleukemia with aberrant self-renewal has not been completely understood.…”

Section: Introductionmentioning

confidence: 99%

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A FOXO1-induced oncogenic network defines the AML1-ETO preleukemic program

Lin

Ptasińska

Rothenberg

et al. 2017

Blood

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Understanding and blocking the self-renewal pathway of preleukemia stem cells could prevent acute myeloid leukemia (AML) relapse. In this study, we show that increased FOXO1 represents a critical mechanism driving aberrant self-renewal in preleukemic cells expressing the t(8;21)-associated oncogene AML1-ETO (AE). Although generally considered as a tumor suppressor, FOXO1 is consistently upregulated in t(8;21) AML. Expression of FOXO1 in human CD34 cells promotes a preleukemic state with enhanced self-renewal and dysregulated differentiation. The DNA binding domain of FOXO1 is essential for these functions. FOXO1 activates a stem cell molecular signature that is also present in AE preleukemia cells and preserved in t(8;21) patient samples. Genome-wide binding studies show that AE and FOXO1 share the majority of their binding sites, whereby FOXO1 binds to multiple crucial self-renewal genes and is required for their activation. In agreement with this observation, genetic and pharmacological ablation of FOXO1 inhibited the long-term proliferation and clonogenicity of AE cells and t(8;21) AML cell lines. Targeting of FOXO1 therefore provides a potential therapeutic strategy for elimination of stem cells at both preleukemic and leukemic stages.

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Section: Plasmids and Reagentsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A FOXO1-induced oncogenic network defines the AML1-ETO preleukemic program

Lin

Ptasińska

Rothenberg

et al. 2017

Blood

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“…Mouse models of AML1-ETO-induced leukemogenesis require a truncated protein that is dramatically diminished in its ability to mediate repression (see ∆NH4 and W692A in Fig. 4), and therefore, may not be reflective of the transcriptional networks established by AML1-ETO in human disease 54 . Thus, we turned to long-term cultures of CD34 + cells from human cord blood to establish a pre-leukemic system to study AML1-ETO transcription functions.…”

Section: Rapid Loss Of Self-renewal and Differentiation Upon Degradatmentioning

confidence: 99%

Definition of a Small Core Transcriptional Circuit Regulated by AML1-ETO

Stengel¹,

Ellis²,

Spielman³

et al. 2020

Preprint

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Transcription factors regulate gene networks controlling normal hematopoiesis and are frequently deregulated in acute myeloid leukemia (AML). Critical to our understanding of the mechanism of cellular transformation by oncogenic transcription factors is the ability to define their direct gene targets. While this seems to be a straight forward task, gene network cascades can change within minutes to hours, making it difficult to distinguish direct from secondary or compensatory transcriptional changes by traditional methodologies. We describe an approach utilizing CRISPR-based genome editing to insert a degron tag into the endogenous AML1-ETO locus of Kasumi-1 cells, as well as overexpression of a degradable AML1-ETO protein in CD34 + human cord blood cells, which is a an AML1-ETO-dependent pre-leukemia model. Upon addition of a small molecule proteolysis targeting chimera (PROTAC), the AML1-ETO protein was rapidly degraded in both systems. Furthermore, by combining rapid degradation with nascent transcript analysis (PRO-seq), RNA-seq and Cut&Run, we have defined the core AML1-ETO regulatory network, which consists of fewer than 100 direct gene targets. The ability of AML1-ETO to regulate this relatively small gene pool is critical for maintaining cells in a selfrenewing state, and AML1-ETO degradation set off a cascade of transcriptional events resulting in myeloid differentiation.

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“…Wang et al. found median survival in leukemic mouse models was increased via inhibition of the lysine acetyltransferase p300 (Wang et al., 2011), which reduced Lys 43 acetylation levels in AML1-ETO9a, a splice isoform of AML1-ETO (Zhang et al., 2007; Link et al., 2016). Though p300 knockdown leads to decreased acetylation, the therapeutic effects of p300 knockdown could be due to effects largely unrelated to AML1-ETO9a acetylation, indicating p300 may be a broader therapeutic target (Wang et al., 2011).…”

Section: T(8;21)mentioning

confidence: 99%

Epigenetic Modifications in Acute Myeloid Leukemia: Prognosis, Treatment, and Heterogeneity

et al. 2019

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Leukemia, specifically acute myeloid leukemia (AML), is a common malignancy that can be differentiated into multiple subtypes based on leukemogenic history and etiology. Although genetic aberrations, particularly cytogenetic abnormalities and mutations in known oncogenes, play an integral role in AML development, epigenetic processes have been shown as a significant and sometimes independent dynamic in AML pathophysiology. Here, we summarize how tumors evolve and describe AML through an epigenetic lens, including discussions on recent discoveries that include prognostics from epialleles, changes in RNA function for hematopoietic stem cells and the epitranscriptome, and novel epigenetic treatment options. We further describe the limitations of treatment in the context of the high degree of heterogeneity that characterizes acute myeloid leukemia.

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Supraphysiologic levels of the AML1-ETO isoform AE9a are essential for transformation

Cited by 14 publications

References 47 publications

A FOXO1-induced oncogenic network defines the AML1-ETO preleukemic program

A FOXO1-induced oncogenic network defines the AML1-ETO preleukemic program

Definition of a Small Core Transcriptional Circuit Regulated by AML1-ETO

Epigenetic Modifications in Acute Myeloid Leukemia: Prognosis, Treatment, and Heterogeneity

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