Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:4.1.99.3 (
PRE
)
1,923
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The glucocorticoid receptor (GR) and the progestin receptor (PR) bind specifically to a variety of DNA sequences, glucocorticoid/progestin response elements (GRE/
PRE
), located in the proximity of responsive gene promoters. Using the isolated recombinant GR DNA-binding domain (DBD), it has recently been shown that GR interacts with the GRE/
PRE
, a 15-basepair partially palindromic consensus sequence, as a dimer. In this study an investigation into the GR-GRE/
PRE
and PR-GRE/
PRE
interaction has been performed using missing base contact analysis with the
tyrosine aminotransferase
GREII (TATII) and recombinant GR DBD as well as a fusion protein consisting of the PR DBD fused to Staph. aureus protein-A. GR and PR had identical base contact points, localized within two consecutive major grooves, binding to the same face of the DNA. Ethylation interference was also performed on the GR DBD-TATII interaction. The contact points with the backbone phosphate groups flank the contacts within the major groove for each of the two half-sites. Knowledge of the contact points within the DNA sequence together with the three-dimensional structure of the protein enables modelling of the protein-DNA interaction.
...
PMID:Identification of protein contact sites within the glucocorticoid/progestin response element. 192 92
We demonstrated previously that two molecules of steroid hormone receptor bound efficiently to a single hormone response element (GRE/
PRE
) of the
tyrosine aminotransferase
gene (Tsai et al., 1988). Here, we show that two tandemly linked GRE/PREs conferred progesterone inducibility synergistically to a heterologous TK-CAT fusion gene. Binding studies demonstrated that occupation of one GRE/
PRE
site by a progesterone receptor dimer increased the binding affinity of receptors for the second GRE/
PRE
site 100-fold. Thus, the observed synergistic induction of TK-CAT may result from cooperative binding of receptor dimers to the two GRE/
PRE
sites.
...
PMID:Cooperative binding of steroid hormone receptors contributes to transcriptional synergism at target enhancer elements. 256 84
The glucocorticoid-progesterone responsive element (GRE/
PRE
) of the
tyrosine aminotransferase
(
TAT
) gene is a steroid-inducible enhancer. We show that the GRE/
PRE
can also work in the absence of a distal promoter element when located 5' to the ovalbumin TATA box. The GRE/
PRE
in this position retains progesterone or glucocorticoid receptor and hormone dependency for the induction of gene expression. Initiation of transcription occurs correctly, and induction occurs at the mRNA level. These data indicate that a steroid-inducible enhancer can function without a distal promoter element.
...
PMID:A steroid response element can function in the absence of a distal promoter. 290 64
