Literature DB >> 11588024

Estrogen-dependent E2a/Pbx1 myeloid cell lines exhibit conditional differentiation that can be arrested by other leukemic oncoproteins.

D B Sykes1, M P Kamps.   

Abstract

The molecular pathways of normal myeloid differentiation, as well as the mechanisms by which oncogenes disrupt this process, remain poorly understood. A major limitation in approaching this problem has been the lack of suitable cell lines that exhibit normal, terminal, and synchronous differentiation in the absence of endogenous oncoproteins and in response to physiologic cytokines, and whose differentiation can be arrested by ectopically expressed human oncoproteins. This report describes clonal, granulocyte-macrophage colony-stimulating factor-dependent myeloid cell lines that exhibit these properties. The cell lines were established by conditional immortalization of primary murine marrow progenitors with an estrogen-regulated E2a/Pbx1-estrogen receptor fusion protein. Clones were identified that proliferated as immortalized blasts in the presence of estrogen, and that exhibited granulocytic, monocytic, or bipotential (granulocytic and monocytic) differentiation on estrogen withdrawal. Differentiation was normal and terminal as evidenced by morphology, cell surface markers, gene expression, and functional assays. The differentiation of the cells could be arrested by heterologous oncoproteins including AML1/ETO, PML/RARalpha, PLZF/RARalpha, Nup98/HoxA9, and other Hox proteins. Furthermore, the study examined the effects of cooperating oncoproteins such as Ras or Bcr/Abl, which allowed for both factor-independent proliferation and differentiation, or Bcl-2, which permitted factor-independent survival but not proliferation. These myeloid cell lines provide tools for examining the biochemical and genetic pathways that accompany normal differentiation as well as a system in which to dissect how other leukemic oncoproteins interfere with these pathways.

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Year:  2001        PMID: 11588024     DOI: 10.1182/blood.v98.8.2308

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  12 in total

1.  Quantitative expansion of ES cell-derived myeloid progenitors capable of differentiating into macrophages.

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Journal:  J Leukoc Biol       Date:  2006-12-08       Impact factor: 4.962

2.  New insights into transcriptional and leukemogenic mechanisms of AML1-ETO and E2A fusion proteins.

Authors:  Jian Li; Chun Guo; Nickolas Steinauer; Jinsong Zhang
Journal:  Front Biol (Beijing)       Date:  2016-09-03

3.  Oxidative metabolism and PGC-1beta attenuate macrophage-mediated inflammation.

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4.  TLX1/HOX11-induced hematopoietic differentiation blockade.

Authors:  I Riz; S S Akimov; S S Eaker; K K Baxter; H J Lee; L Mariño-Ramírez; D Landsman; T S Hawley; R G Hawley
Journal:  Oncogene       Date:  2007-01-08       Impact factor: 9.867

5.  Meis1 programs transcription of FLT3 and cancer stem cell character, using a mechanism that requires interaction with Pbx and a novel function of the Meis1 C-terminus.

Authors:  Gang G Wang; Martina P Pasillas; Mark P Kamps
Journal:  Blood       Date:  2005-03-08       Impact factor: 22.113

6.  E2a/Pbx1 induces the rapid proliferation of stem cell factor-dependent murine pro-T cells that cause acute T-lymphoid or myeloid leukemias in mice.

Authors:  David B Sykes; Mark P Kamps
Journal:  Mol Cell Biol       Date:  2004-02       Impact factor: 4.272

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8.  Retrovirus-Mediated Expression of E2A-PBX1 Blocks Lymphoid Fate but Permits Retention of Myeloid Potential in Early Hematopoietic Progenitors.

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Journal:  PLoS One       Date:  2015-06-22       Impact factor: 3.240

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Authors:  Alex Hopke; Allison Scherer; Samantha Kreuzburg; Michael S Abers; Christa S Zerbe; Mary C Dinauer; Michael K Mansour; Daniel Irimia
Journal:  Nat Commun       Date:  2020-04-27       Impact factor: 14.919

10.  Differential ACPA Binding to Nuclear Antigens Reveals a PAD-Independent Pathway and a Distinct Subset of Acetylation Cross-Reactive Autoantibodies in Rheumatoid Arthritis.

Authors:  Katy A Lloyd; Gustaf Wigerblad; Peter Sahlström; Manasa G Garimella; Karine Chemin; Johanna Steen; Philip J Titcombe; Bianka Marklein; Diana Zhou; Ragnhild Stålesen; Elena Ossipova; Christina Lundqvist; Olov Ekwall; Johan Rönnelid; Daniel L Mueller; Mikael C I Karlsson; Mariana J Kaplan; Karl Skriner; Lars Klareskog; Fredrik Wermeling; Vivianne Malmström; Caroline Grönwall
Journal:  Front Immunol       Date:  2019-01-04       Impact factor: 7.561

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