PROENKEPHALIN GENE-EXPRESSION - INTERACTION OF GLUCOCORTICOID AND CAMP REGULATORY ELEMENTS

被引：11

作者：

JENAB, S

INTURRISI, CE

机构：

[1] Department of Pharmacology, Cornell University Medical College, New York

来源：

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS | 1995年 / 210卷 / 02期

关键词：

D O I：

10.1006/bbrc.1995.1700

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

We used gel shift assays to determine the affinities of a 15 base glucocorticoid response element (GRE) derived from the rat proenkephalin (Penk) gene for the glucocorticoid receptor. A DNA binding domain of the glucocorticoid receptor interacted with a rat GRE (RGRE) with an apparent affinity intermediate between that of a consensus positive GRE oligo (GRE+) and a mismatch GRE oligo (GRE-). When inserted in front of a chloramphenicol acyl transferase (CAT) construct that is driven by a Penk promoter containing a cAMP response element, dexamethasone (10 mu M) produced a 5-fold increase with GRE+, a small increase with RGRE, and no change with GRE- or the Penk promoter alone. Forskolin (20 mu M) stimulated CAT activity 4- to 9-fold with each construct. However, dexamethasone plus forskolin caused a synergistic induction of CAT expression with the GRE+ oligo, no effect with the RGRE and an antagonistic effect with the Penk promoter alone and the GRE- oligo, These results demonstrate that GRE+, and to a lesser degree RGRE, can mimic the response of the endogenous Penk gene to dexamethasone and forskolin. Furthermore, a dexamethasone activated glucocorticoid receptor may inhibit cAMP mediated transcription of the Penk gene when a GRE+ or RGRE is not present. (C) 1995 Academic Press. Inc.

引用

页码：589 / 599

页数：11

共 30 条

[1] NEGATIVE REGULATION BY GLUCOCORTICOIDS THROUGH INTERFERENCE WITH A CAMP RESPONSIVE ENHANCER
AKERBLOM, IE
SLATER, EP
BEATO, M
BAXTER, JD
MELLON, PL
[J]. SCIENCE, 1988, 241 (4863) : 350 - 353
[2] LIGAND-DEPENDENT CONFORMATIONAL-CHANGES IN THE PROGESTERONE-RECEPTOR ARE NECESSARY FOR EVENTS THAT FOLLOW DNA-BINDING
ALLAN, GF
TSAI, SY
TSAI, MJ
OMALLEY, BW
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (24) : 11750 - 11754
[3] DNA-BINDING ANALYSIS OF GLUCOCORTICOID RECEPTOR SPECIFICITY MUTANTS
ALROY, I
FREEDMAN, LP
[J]. NUCLEIC ACIDS RESEARCH, 1992, 20 (05) : 1045 - 1052
[4] A CYCLIC AMP- AND PHORBOL ESTER-INDUCIBLE DNA ELEMENT
COMB, M
BIRNBERG, NC
SEASHOLTZ, A
HERBERT, E
GOODMAN, HM
[J]. NATURE, 1986, 323 (6086) : 353 - 356
[5] PRIMARY STRUCTURE OF THE HUMAN PROENKEPHALIN GENE
COMB, M
ROSEN, H
SEEBURG, P
ADELMAN, J
HERBERT, E
[J]. DNA-A JOURNAL OF MOLECULAR & CELLULAR BIOLOGY, 1983, 2 (03): : 213 - 229
[6] COMB M, 1991, MOL APPROACHES DRUG, V1, P149
[7] TRANSCRIPTION FACTOR INTERACTIONS - SELECTORS OF POSITIVE OR NEGATIVE REGULATION FROM A SINGLE DNA ELEMENT
DIAMOND, MI
MINER, JN
YOSHINAGA, SK
YAMAMOTO, KR
[J]. SCIENCE, 1990, 249 (4974) : 1266 - 1272
[8] GLUCOCORTICOID RECEPTOR-BINDING TO A SPECIFIC DNA-SEQUENCE IS REQUIRED FOR HORMONE-DEPENDENT REPRESSION OF PRO-OPIOMELANOCORTIN GENE-TRANSCRIPTION
DROUIN, J
TRIFIRO, MA
PLANTE, RK
NEMER, M
ERIKSSON, P
WRANGE, O
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (12) : 5305 - 5314
[9] NOVEL GLUCOCORTICOID RECEPTOR COMPLEX WITH DNA ELEMENT OF THE HORMONE-REPRESSED POMC GENE
DROUIN, J
SUN, YL
CHAMBERLAND, M
GAUTHIER, Y
DELEAN, A
NEMER, M
SCHMIDT, TJ
[J]. EMBO JOURNAL, 1993, 12 (01) : 145 - 156
[10] THE FUNCTION AND STRUCTURE OF THE METAL COORDINATION SITES WITHIN THE GLUCOCORTICOID RECEPTOR DNA-BINDING DOMAIN
FREEDMAN, LP
LUISI, BF
KORSZUN, ZR
BASAVAPPA, R
SIGLER, PB
YAMAMOTO, KR
[J]. NATURE, 1988, 334 (6182) : 543 - 546

← 1 2 3 →