Functional analysis of the homeodomain protein SIX5

doi:10.1093/nar/28.9.1871

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Nucleic Acids Research, 2000, Vol. 28, No. 9 1871-1878
© 2000 Oxford University Press

Functional analysis of the homeodomain protein SIX5

Sarah E. Harris, Catherine L. Winchester and Keith J. Johnson^*

Division of Molecular Genetics, Institute of Biomedical and Life Sciences, University of Glasgow, Anderson College, 56 Dumbarton Road, Glasgow G11 6NU, UK

SIX5 (previously known as myotonic dystrophy associated homeodomainprotein-DMAHP) is a member of the SIX [sine oculis homeobox(Drosophila) homologue] gene family which encodes proteins containinga SIX domain adjacent to a homeodomain. To investigatethe DNA binding specificities of these two domains in SIX5,they were expressed as GST fusion proteins, both separatelyand together. Affinity purified recombinant proteins and celllysates from bacteria expressing the recombinant proteins wereused in gel retardation assays with double stranded oligonucleotidesrepresenting putative DNA binding sites. The putative sitesincluded two in the promoter region of DMPK (dystrophia myotonicaprotein kinase) and the previously characterised murine Six4DNA binding site in the Na⁺/K⁺ ATPase ${alpha}$ 1 subunit gene (ATP1A1)regulatory element (ARE). None of the recombinant proteins showedany affinity for the two putative sites in DMPK. However, thetwo recombinant proteins containing the homeodomain both formedat least one specific complex with the ARE. The recombinantprotein containing both domains formed a second specific complexwith the ARE, assumed to be a dimer complex. Finally, a wholegenome PCR-based screen was used to identify genomic DNA sequencesto which SIX5 binds, as an initial stage in the identificationof genes regulated by SIX5.

^* To whom correspondence should be addressed. Tel: +44 141 3305101; Fax: +44 141 330 6871; Email: k.johnson@bio.gla.ac.uk

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