Literature DB >> 7555717

The Hox11 gene is essential for cell survival during spleen development.

T N Dear1, W H Colledge, M B Carlton, I Lavenir, T Larson, A J Smith, A J Warren, M J Evans, M V Sofroniew, T H Rabbitts.   

Abstract

The HOX11 homeobox gene was identified via the translocation t(10;14) in T cell leukaemia. To determine the function of this gene in mice, null mutations were made using homologous recombination in ES cells to incorporate lacZ into the hox11 transcription unit. Production of beta-galactosidase from the recombinant hox11 allele in +/- mutants allowed identification of sites of hox11 expression which included the developing spleen. Newborn hox11 -/- mice exhibit asplenia. Spleen formation commences normally at E11.5 in hox11 -/- mutant embryos but the spleen anlage undergoes rapid and complete resorption between E12.5 and E13.5. Dying spleen cells exhibit molecular features of apoptosis, suggesting that programmed cell death is initiated at this stage of organ development in the absence of hox11 protein. Thus hox11 is not required to initiate spleen development but is essential for the survival of splenic precursors during organogenesis. This function for hox11 suggests that enhanced cell survival may result from the t(10;14) which activates HOX11 in T cell leukaemias, further strengthening the association between oncogene-induced cell survival and tumorigenesis.

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Year:  1995        PMID: 7555717     DOI: 10.1242/dev.121.9.2909

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  35 in total

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Journal:  EMBO J       Date:  2015-01-19       Impact factor: 11.598

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8.  Proteomics identifies multipotent and low oncogenic risk stem cells of the spleen.

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10.  Comparative genome-wide DNA methylation analysis of colorectal tumor and matched normal tissues.

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Journal:  Epigenetics       Date:  2012-10-18       Impact factor: 4.528

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