Identification of DNA elements cooperatively activating proopiomelanocortin gene expression in the pituitary glands of transgenic mice.

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Mol Cell Biol. 1992 September; 12(9): 3978-3990

Identification of DNA elements cooperatively activating proopiomelanocortin gene expression in the pituitary glands of transgenic mice.

B Liu, G D Hammer, M Rubinstein, M Mortrud and M J Low

Vollum Institute for Advanced Biomedical Research, Oregon Health Sciences University, Portland 97201.

ABSTRACT

The proopiomelanocortin (POMC) gene is highly expressed in adultmouse pituitary anterior lobe corticotrophs and intermediatelobe melanotrophs. To identify the DNA elements important forthis tissue-specific expression, we analyzed a series of POMCreporter genes in transgenic mice. A DNA fragment containingrat POMC 5'-flanking sequences from -323 to -34 recapitulatedboth basal pituitary cell-specific and hormonally stimulatedexpression in adult mice when fused to a heterologous thymidinekinase promoter. Developmental onset of the reporter gene expressionlagged by 1 day but otherwise closely paralleled the normalontogeny of murine POMC gene expression, including corticotrophactivation at embryonic day 14.5 (E14.5) followed by melanotrophactivation at E15.5 to E16.5. AtT20 corticotroph nuclear proteinextracts interacted with three specific regions of the functionalPOMC promoter in DNase I protection assays. The positions ofthese protected sites were -107 to -160 (site 1), -182 to -218(site 2), and -249 to -281 (site 3). Individual deletions ofthese footprinted sites did not alter transgene expression;however, the simultaneous deletion of sites 2 and 3 preventedtransgene expression in both corticotrophs and melanotrophs.Electrophoretic mobility shift and Southwestern (DNA-protein)assays demonstrated that multiple AtT20 nuclear proteins boundto these footprinted sites. We conclude that the sequences between-323 and -34 of the rat POMC gene promoter are both necessaryand sufficient for correct spatial, temporal, and hormonallyregulated expression in the pituitary gland. Our data suggestthat the three footprinted sites within the promoter are functionallyinterchangeable and act in combination with promoter elementsbetween -114 and -34. The inability of any reporter gene constructionto dissociate basal and hormonally stimulated expression suggeststhat these DNA elements are involved in both of these two characteristicsof POMC gene expression in vivo.

Mol Cell Biol. 1992 September; 12(9): 3978-3990

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