High GATA2 expression is a poor prognostic marker in pediatric acute myeloid leukemia

Luesink, Maaike; Hollink, Iris H.I.M.; Velden, Vincent H.J. van der; Knops, Ruth; Boezeman, J.B.M.; Haas, Valérie de; Trka, Jan; Baruchel, André; Reinhardt, Dirk; Reijden, Bert A. van der; Heuvel‐Eibrink, Marry M. van den; Zwaan, C. Michel; Jansen, Joop H.

doi:10.1182/blood-2011-12-397083

Cited by 69 publications

(61 citation statements)

References 51 publications

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“…Consistent with this possibility, GATA2 is overexpressed in the BM of both pediatric and adult acute myeloid leukemia patients, and aberrant GATA2 expression is also observable in leukemic blasts [7][8][9][10]. Patients in remission display GATA2 levels that return to normal, whereas patients with resistant disease display continued GATA2 overexpression [8].…”

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confidence: 76%

Low-level GATA2 overexpression promotes myeloid progenitor self-renewal and blocks lymphoid differentiation in mice

Nandakumar

Johnson

Throm

et al. 2015

Experimental Hematology

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The transcription factor GATA2 is highly expressed in hematopoietic stem cells and is downregulated during lineage maturation. Gain of function mutations, loss of function mutations, and overexpression of GATA2 have been reported in acute myeloid leukemia. In previous studies, we and others showed that GATA2 overexpression at high levels, similar to that seen in hematopoietic stem cells, blocked differentiation of hematopoietic stem cells and progenitors. To better understand the effects of GATA2, we designed a Tamoxifen-inducible GATA2-estrogen receptor (ERT) vector. In the absence of Tamoxifen, small amounts of GATA2-ERT were still able to enter the nucleus in mouse bone marrow (BM) cells, providing us with a tool to test the effects of low-level GATA2 overexpression. We observed that this low-level GATA2 overexpression enhanced self-renewal of myeloid progenitors in vitro and resulted in immortalization of BM cells to myeloid cell lines. Continuous GATA2-ERT expression was required for the proliferation of these immortalized lines. Myeloid expansion and a block in T and B lineage differentiation were observed in mice transplanted with GATA2-ERT-expressing BM cells. Myeloid expansion occurred after the granulocyte monocyte progenitor stage, and lymphoid block was distal to the common lymphoid progenitor in transgenic mice. GATA2 appeared to induce growth via downstream activation of Nmyc and Hoxa9. Our results demonstrate that GATA2 overexpression at low level confers self-renewal capacity to myeloid progenitors and is relevant to myeloid leukemia development.

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confidence: 76%

Low-level GATA2 overexpression promotes myeloid progenitor self-renewal and blocks lymphoid differentiation in mice

Nandakumar

Johnson

Throm

et al. 2015

Experimental Hematology

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“…GATA2 is a key regulator of hematopoietic stem cell 32 and megakaryocyte development, 46 and high GATA2 expression has recently been reported as a poor prognostic factor in pediatric AML. 31 HEY2 is largely recognized as a regulator of 47 but was shown to act upstream of Notch to induce hematopoietic stem cell formation in zebrafish embryos. 33 The involvement of both HEY2 and GATA2 in early hematopoiesis, their increased expression in human AML progenitors, 20 and their overexpression specifically in TgERG myeloid but not lymphoid leukemia (supplemental Figure 9) suggest a role for both transcription factors in sustaining the immature nature of ERGinduced myeloid leukemia.…”

Section: Discussionmentioning

confidence: 99%

“…GATA2 is an important regulator early in hematopoiesis and is perturbed in hematologic malignancies. [30][31][32] Moreover, ERG was shown to be a direct upstream regulator of GATA2 during the second wave of hematopoiesis. 2 Involvement of the bHLH transcription factor Hey2 in hematopoietic stem cell specification in zebrafish has been recently suggested.…”

Section: Integrated Genomic Analysis Reveals An Erg-regulated Transcrmentioning

confidence: 99%

Genome-scale expression and transcription factor binding profiles reveal therapeutic targets in transgenic ERG myeloid leukemia

Goldberg

Tijssen

Birger

et al. 2013

Blood

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Key Points• ERG overexpression in transgenic mice induces a transcriptional leukemia stem cell program characteristic of human AML. • PIM1 and RAS are relevant ERG therapeutic targets.The ETS transcription factor ERG plays a central role in definitive hematopoiesis, and its overexpression in acute myeloid leukemia (AML) is associated with a stem cell signature and poor prognosis. Yet how ERG causes leukemia is unclear. Here we show that panhematopoietic ERG expression induces an early progenitor myeloid leukemia in transgenic mice. Integrated genome-scale analysis of gene expression and ERG binding profiles revealed that ERG activates a transcriptional program similar to human AML stem/ progenitor cells and to human AML with high ERG expression. This transcriptional program was associated with activation of RAS that was required for leukemia cells growth in vitro and in vivo. We further show that ERG induces expression of the Pim1 kinase oncogene through a novel hematopoietic enhancer validated in transgenic mice and human CD341 normal and leukemic cells. Pim1 inhibition disrupts growth and induces apoptosis of ERG-expressing leukemic cells.The importance of the ERG/PIM1 axis is further underscored by the poorer prognosis of AML highly expressing ERG and PIM1. Thus, integrative genomic analysis demonstrates that ERG causes myeloid progenitor leukemia characterized by an induction of leukemia stem cell transcriptional programs. Pim1 and the RAS pathway are potential therapeutic targets of these high-risk leukemias. (Blood. 2013;122(15):2694-2703

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“…The incidence in unselected cases of MDS or AML is actually quite low, at <5%, and may include cases of GATA2 germ-line mutation that were assumed to be somatic, in the absence of a germ-line DNA control (Yan et al, 2011;Luesink et al, 2012;Papaemmanuil et al, 2013;Shiba et al, 2014). Gain of function mutation L359V has been documented in blast transformation of CML, associated with typically poor outlook (Zhang et al, 2008(Zhang et al, , 2009.…”

Section: Acquired Genetic Abnormalities and Evolution To Leukaemiamentioning

confidence: 99%

Haematopoietic and immune defects associated with GATA2 mutation

Collin

2018

Pathology

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SummaryHeterozygous familial or sporadic GATA2 mutations cause a multifaceted disorder, encompassing susceptibility to infection, pulmonary dysfunction, autoimmunity, lymphoedema and malignancy. Although often healthy in childhood, carriers of defective GATA2 alleles develop progressive loss of mononuclear cells (dendritic cells, monocytes, B and Natural Killer lymphocytes), elevated FLT3 ligand, and a 90% risk of clinical complications, including progression to myelodysplastic syndrome (MDS) by 60 years of age. Premature death may occur from childhood due to infection, pulmonary dysfunction, solid malignancy and MDS/acute myeloid leukaemia. GATA2 mutations include frameshifts, amino acid substitutions, insertions and deletions scattered throughout the gene but concentrated in the region encoding the two zinc finger domains. Mutations appear to cause haplo-insufficiency, which is known to impair haematopoietic stem cell survival in animal models. Management includes genetic counselling, prevention of infection, cancer surveillance, haematopoietic monitoring and, ultimately, stem cell transplantation upon the development of MDS or another lifethreatening complication.

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High GATA2 expression is a poor prognostic marker in pediatric acute myeloid leukemia

Cited by 69 publications

References 51 publications

Low-level GATA2 overexpression promotes myeloid progenitor self-renewal and blocks lymphoid differentiation in mice

Low-level GATA2 overexpression promotes myeloid progenitor self-renewal and blocks lymphoid differentiation in mice

Genome-scale expression and transcription factor binding profiles reveal therapeutic targets in transgenic ERG myeloid leukemia

Haematopoietic and immune defects associated with GATA2 mutation

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