TLX1/HOX11 transcription factor inhibits differentiation and promotes a non‐haemopoietic phenotype in murine bone marrow cells

Dixon, Darcelle N.; Izon, David J.; Dagger, Samantha A.; Callow, Matthew J.; Taplin, Ross; Kees, Ursula R.; Greene, Wayne K.

doi:10.1111/j.1365-2141.2007.06626.x

Cited by 14 publications

(14 citation statements)

References 69 publications

(131 reference statements)

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“…These included Ccna2, Ccnb1, Ccnb2, Cdc20 [14,16], Cdc25a [26], Cdc6, Mcm2, Mcm4, Mcm5, Mcm6, Rad51, Top2a and Ttk [24]. To this set, we added TLX1 ChIP-chip targets that were shown to be directly activated by CUX1 and relevant to the establishment of bipolar mitoses leading to CIN (Aurkb, Bub1, Bub3, Camk2d, Cenpa, Cenpe, Kifc1, Kif2c, Mad2l1, Nek2, Ttk and Zw10) [73].…”

Section: Resultsmentioning

confidence: 99%

The DN2 Myeloid-T (DN2mt) Progenitor is a Target Cell for Leukemic Transformation by the TLX1 Oncogene

et al. 2013

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Introduction Inappropriate activation of the TLX1 (T-cell leukemia homeobox 1) gene by chromosomal translocation is a recurrent event in human T-cell Acute Lymphoblastic Leukemia (T-ALL). Ectopic expression of TLX1 in murine bone marrow progenitor cells using a conventional retroviral vector efficiently yields immortalized cell lines and induces T-ALL-like tumors in mice after long latency. Methods To eliminate a potential contribution of retroviral insertional mutagenesis to TLX1 immortalizing and transforming function, we incorporated the TLX1 gene into an insulated self-inactivating retroviral vector. Results Retrovirally transduced TLX1-expressing murine bone marrow progenitor cells had a growth/survival advantage and readily gave rise to immortalized cell lines. Extensive characterization of 15 newly established cell lines failed to reveal a common retroviral integration site. This comprehensive analysis greatly extends our previous study involving a limited number of cell lines, providing additional support for the view that constitutive TLX1 expression is sufficient to initiate the series of events culminating in hematopoietic progenitor cell immortalization. When TLX1-immortalized cells were co-cultured on OP9-DL1 monolayers under conditions permissive for T-cell differentiation, a latent T-lineage potential was revealed. However, the cells were unable to transit the DN2 myeloid-T (DN2mt)-DN2 T-lineage determined (DN2t) commitment step. The differentiation block coincided with failure to upregulate the zinc finger transcription factor gene Bcl11b, the human ortholog of which was shown to be a direct transcriptional target of TLX1 downregulated in the TLX1+ T-ALL cell line ALL-SIL. Other studies have described the ability of TLX1 to promote bypass of mitotic checkpoint arrest, leading to aneuploidy. We likewise found that diploid TLX1-expressing DN2mt cells treated with the mitotic inhibitor paclitaxel bypassed the mitotic checkpoint and displayed chromosomal instability. This was associated with elevated expression of TLX1 transcriptional targets involved in DNA replication and mitosis, including Ccna2 (cyclin A2), Ccnb1 (cyclin B1), Ccnb2 (cyclin B2) and Top2a (topoisomerase IIα). Notably, enforced expression of BCL11B in ALL-SIL T-ALL cells conferred resistance to the topoisomerase IIα poison etoposide. Conclusion Taken together with previous findings, the data reinforce a mechanism of TLX1 oncogenic activity linked to chromosomal instability resulting from dysregulated expression of target genes involved in mitotic processes. We speculate that repression of BCL11B expression may provide part of the explanation for the observation that aneuploid DNA content in TLX1+ leukemic T cells does not necessarily portend an unfavorable prognosis. This TLX1 hematopoietic progenitor cell immortalization/T-cell differentiation assay should help further our understanding of the mechanisms of TLX1-mediated evolution to malignancy and has the potential to be a useful predictor of disease response to novel thera...

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Section: Resultsmentioning

confidence: 99%

The DN2 Myeloid-T (DN2mt) Progenitor is a Target Cell for Leukemic Transformation by the TLX1 Oncogene

et al. 2013

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“…On the other hand, these genes might mimic NKL genes that have a role in normal T-cell development, thereby making use of existing pathways, in line with a 'lineage-survival model'. HHEX 49 and MSX2 67 have both been proposed as candidate genes that might be mimicked by ectopically expressed NKL genes. HHEX is highly expressed in early hematopoietic progenitors and downregulated upon T-cell differentiation.…”

Section: Nkl Overexpression As a Common Theme In T-allmentioning

confidence: 99%

“…In general, NKL genes function predominantly as transcriptional repressors, although activating properties have also been described. 49,102,103 More than half (32/48) of the NKL homeodomain proteins contain a conserved Engrailed homology 1 (Eh1) motif (FxIxxIL, whereby x can be any amino acid) 104,105 at their N terminal (defined here as having at least 3 out of 4 conserved amino acids present at the correct position at the N-terminal side, Table 1). The Eh1 domain functions as a strong transcriptional repressor.…”

Section: Nkls Modes Of Actionmentioning

confidence: 99%

NKL homeobox genes in leukemia

2011

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“…Comparisons of differentially expressed HOX genes revealed Caudal type homeobox 1 (CDX1), T-cell leukemia homeobox 1 (TLX1), and HOXD3 among the most significantly decreased in both FANCAi and FANCD2i day 20 EBs (Figure 6G). CDX1 and TLX1 have known roles in hematopoietic specification and progenitor proliferation, 43,44 whereas HOXD3 has been shown to play a role in patterning the anterior-posterior axis and the embryonic skeleton. 45 In addition to their role in tissue specification, HOX genes have been shown to directly influence the cell cycle machinery and cellular proliferation.…”

Section: Fa Gene Complementation Rescues Hematopoietic Deficitsmentioning

confidence: 99%

Knockdown of Fanconi anemia genes in human embryonic stem cells reveals early developmental defects in the hematopoietic lineage

Tulpule

Lensch

Miller

et al. 2010

Blood

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TLX1/HOX11 transcription factor inhibits differentiation and promotes a non‐haemopoietic phenotype in murine bone marrow cells

Cited by 14 publications

References 69 publications

The DN2 Myeloid-T (DN2mt) Progenitor is a Target Cell for Leukemic Transformation by the TLX1 Oncogene

The DN2 Myeloid-T (DN2mt) Progenitor is a Target Cell for Leukemic Transformation by the TLX1 Oncogene

NKL homeobox genes in leukemia

Knockdown of Fanconi anemia genes in human embryonic stem cells reveals early developmental defects in the hematopoietic lineage

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