Literature DB >> 8980258

Properties of the mouse alpha-globin HS-26: relationship to HS-40, the major enhancer of human alpha-globin gene expression.

E E Bouhassira1, M F Kielman, J Gilman, M F Fabry, S Suzuka, O Leone, E Gikas, L F Bernini, R L Nagel.   

Abstract

HS-26, the mouse homologue of HS-40, is the major regulatory element of the mouse alpha-globin gene locus. Like HS-40, HS-26 is located within an intron of a house-keeping gene; comparison of the nucleotide sequences of HS-26 and HS-40 reveals conservation of the sequences and positions of several DNA binding motifs in the 5' regions of both elements (3 GATA, 2 NFE-2, and 1 CACCC sites) and the absence in HS-26 of three CACCC sites and one GATA site that are present in the 3' region of HS-40, suggesting that the two elements might not be identical. We report here that when HS-26 is linked to a 1.5 kb Pstl human alpha-globin gene fragment, it has a weak enhancer activity in induced MEL cells and in transgenic embryos, and it does not have any detectable activity in adult transgenic mice. This suggests that HS-26 does not have Locus Control Region (LCR) activity but can act as an enhancer during the embryonic life when integrated at a permissive locus. To further test the importance of HS-26 at its natural locus, we have generated embryonic stem cells and chimeric animals in which 350 bp containing HS-26 have been replaced by a neomycin resistance gene by homologous recombination. The sizes of the chimeras' red cells were then estimated by measuring forward scattering on a FacsScan apparatus in hypotonic conditions. This revealed that a fraction of the chimeric animals' red cells were smaller than normal mouse red cells and were very similar to cells from mice heterozygous for alpha-thalassemia. Density gradient analysis also suggested the presence of thalassemic cells. These results indicated that despite its lack of LCR activity, HS-26 is important for the regulation of the mouse alpha-globin gene locus.

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Year:  1997        PMID: 8980258     DOI: 10.1002/(sici)1096-8652(199701)54:1<30::aid-ajh5>3.0.co;2-5

Source DB:  PubMed          Journal:  Am J Hematol        ISSN: 0361-8609            Impact factor:   10.047


  5 in total

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Authors:  Alister P W Funnell; Douglas Vernimmen; Wooi F Lim; Ka Sin Mak; Beeke Wienert; Gabriella E Martyn; Crisbel M Artuz; Jon Burdach; Kate G R Quinlan; Douglas R Higgs; Emma Whitelaw; Richard C M Pearson; Merlin Crossley
Journal:  BMC Mol Biol       Date:  2014-05-16       Impact factor: 2.946

  5 in total

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