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

Woodcroft, Mark W.; Nanan, Kyster K.; Thompson, Patrick; Tyryshkin, Kathrin; Smith, Steven P.; Slany, Robert K.; LeBrun, David P.

doi:10.1371/journal.pone.0130495

Cited by 3 publications

(1 citation statement)

References 53 publications

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“…Unexpectedly, in experimental models designed to study the mechanism by which E2a-Pbx1 induces leukemia, retroviral mediated expression of E2a-Pbx1 in hematopoietic progenitors gives rise to myeloid, not lymphoid leukemia. The work of Woodcroft [ 71 ] et al, has clarified this puzzle by showing that the neoplastic phenotype depends on the developmental stage of the cell into which the oncoprotein is introduced. E2a-Pbx1 appears to function as a dominant negative mutation of E2A which, when introduced in early progenitors induces a complete block prior to the CLP stage.…”

Section: Introductionmentioning

confidence: 99%

The telomere complex and the origin of the cancer stem cell

Torres-Montaner

2021

Biomark Res

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Exquisite regulation of telomere length is essential for the preservation of the lifetime function and self-renewal of stem cells. However, multiple oncogenic pathways converge on induction of telomere attrition or telomerase overexpression and these events can by themselves trigger malignant transformation. Activation of NFκB, the outcome of telomere complex damage, is present in leukemia stem cells but absent in normal stem cells and can activate DOT1L which has been linked to MLL-fusion leukemias. Tumors that arise from cells of early and late developmental stages appear to follow two different oncogenic routes in which the role of telomere and telomerase signaling might be differentially involved. In contrast, direct malignant transformation of stem cells appears to be extremely rare. This suggests an inherent resistance of stem cells to cancer transformation which could be linked to a stem cell’specific mechanism of telomere maintenance. However, tumor protection of normal stem cells could also be conferred by cell extrinsic mechanisms.

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Section: Introductionmentioning

confidence: 99%

The telomere complex and the origin of the cancer stem cell

Torres-Montaner

2021

Biomark Res

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Oncogenesis by E2A-PBX1 in ALL: RUNX and more

Licht

2020

Blood

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E2A regulates neural ectoderm fate specification in human embryonic stem cells

Huang

Zhou

et al. 2020

Development

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E proteins transcription factors are critical for many cell fate decisions. However, the roles of E proteins in the germ-layer specification of human embryonic stem cells (hESC) are poorly understood. We disrupted the TCF3 gene locus to delete the E protein E2A in hESCs. E2A KO hESCs retained key features of pluripotency, but displayed decreased neural ectoderm coupled with enhanced mesoendoderm outcomes. Genome-wide analyses showed that E2A directly regulates neural ectoderm and Nodal pathway genes. Accordingly, inhibition of Nodal or E2A overexpression partially rescued the neural ectoderm defect in E2A KO hESCs. Loss of E2A had little impact on the epigenetic landscape of hESCs, whereas E2A KO neural precursors displayed increased accessibility of the gene locus encoding the Nodal agonist CRIPTO. Double-deletion of both E2A and HEB (TCF12) resulted in a more severe neural ectoderm defect. Therefore, this study reveals critical context-dependent functions for E2A in human neural ectoderm fate-specification.

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

Cited by 3 publications

References 53 publications

The telomere complex and the origin of the cancer stem cell

The telomere complex and the origin of the cancer stem cell

Oncogenesis by E2A-PBX1 in ALL: RUNX and more

E2A regulates neural ectoderm fate specification in human embryonic stem cells

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