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CHARACTERIZATION OF THE MOUSE JUND PROMOTER - HIGH BASAL LEVEL ACTIVITY DUE TO AN OCTAMER MOTIF

被引:54
作者
DEGROOT, RP [1 ]
KARPERIEN, M [1 ]
PALS, C [1 ]
KRUIJER, W [1 ]
机构
[1] NETHERLANDS INST DEV BIOL,HUBRECHT LAB,3584 CT UTRECHT,NETHERLANDS
来源
EMBO JOURNAL | 1991年 / 10卷 / 09期
关键词
JUN; OCTAMER; TRE; TRANSCRIPTION REGULATION;
D O I
10.1002/j.1460-2075.1991.tb07792.x
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
The product of the junD gene belongs to the Jun/Fos family of nuclear DNA binding transcription factors. This family regulates the expression of TPA responsive genes by binding to the TPA responsive element (TRE). Unlike its counterparts c-jun and junB, junD expression is hardly inducible by growth factors and phorbol esters. In fact, junD is constitutively expressed at high levels in a wide variety of cells. To unravel the molecular mechanisms underlying constitutive junD expression, we have cloned and characterized the mouse junD promoter. We show that the high constitutive expression is caused by multiple cis-acting elements in its promoter, including an SP1 binding site, an octamer motif, a CAAT box, a Zif268 binding site and a TRE-like sequence. The octamer motif is the major determinant of junD promoter activity, while somewhat smaller contributions are made by the TRE and Zif268 binding site. The SP1 and CAAT box are shown to be of minor importance. The junD TRE is in its behavior indistinguishable from previously identified TREs. However, the junD promoter is not TPA inducible due to the presence of the octamer motif.
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页码:2523 / 2532
页数:10
相关论文
共 72 条
[1]   THE JUN PROTO-ONCOGENE IS POSITIVELY AUTOREGULATED BY ITS PRODUCT, JUN/AP-1 [J].
ANGEL, P ;
HATTORI, K ;
SMEAL, T ;
KARIN, M .
CELL, 1988, 55 (05) :875-885
[2]   12-O-TETRADECANOYL-PHORBOL-13-ACETATE INDUCTION OF THE HUMAN COLLAGENASE GENE IS MEDIATED BY AN INDUCIBLE ENHANCER ELEMENT LOCATED IN THE 5'-FLANKING REGION [J].
ANGEL, P ;
BAUMANN, I ;
STEIN, B ;
DELIUS, H ;
RAHMSDORF, HJ ;
HERRLICH, P .
MOLECULAR AND CELLULAR BIOLOGY, 1987, 7 (06) :2256-2266
[3]   ONCOGENE JUN ENCODES A SEQUENCE-SPECIFIC TRANS-ACTIVATOR SIMILAR TO AP-1 [J].
ANGEL, P ;
ALLEGRETTO, EA ;
OKINO, ST ;
HATTORI, K ;
BOYLE, WJ ;
HUNTER, T ;
KARIN, M .
NATURE, 1988, 332 (6160) :166-171
[4]   PHORBOL ESTER INDUCIBLE GENES CONTAIN A COMMON CIS ELEMENT RECOGNIZED BY A TPA-MODULATED TRANS-ACTING FACTOR [J].
ANGEL, P ;
IMAGAWA, M ;
CHIU, R ;
STEIN, B ;
IMBRA, RJ ;
RAHMSDORF, HJ ;
JONAT, C ;
HERRLICH, P ;
KARIN, M .
CELL, 1987, 49 (06) :729-739
[5]   DISTINCT FACTORS WITH SP1 AND NF-A SPECIFICITIES BIND TO ADJACENT FUNCTIONAL ELEMENTS OF THE HUMAN U2 SNRNA GENE ENHANCER [J].
ARES, M ;
CHUNG, JS ;
GIGLIO, L ;
WEINER, AM .
GENES & DEVELOPMENT, 1987, 1 (08) :808-817
[6]   COUPLED AND UNCOUPLED INDUCTION OF FOS AND JUN TRANSCRIPTION BY DIFFERENT 2ND MESSENGERS IN CELLS OF HEMATOPOIETIC ORIGIN [J].
AUWERX, J ;
STAELS, B ;
SASSONECORSI, P .
NUCLEIC ACIDS RESEARCH, 1990, 18 (02) :221-228
[7]   GROWTH-FACTORS AND MEMBRANE DEPOLARIZATION ACTIVATE DISTINCT PROGRAMS OF EARLY RESPONSE GENE-EXPRESSION - DISSOCIATION OF FOS AND JUN INDUCTION [J].
BARTEL, DP ;
SHENG, M ;
LAU, LF ;
GREENBERG, ME .
GENES & DEVELOPMENT, 1989, 3 (03) :304-313
[8]   HUMAN PROTOONCOGENE C-JUN ENCODES A DNA-BINDING PROTEIN WITH STRUCTURAL AND FUNCTIONAL-PROPERTIES OF TRANSCRIPTION FACTOR AP-1 [J].
BOHMANN, D ;
BOS, TJ ;
ADMON, A ;
NISHIMURA, T ;
VOGT, PK ;
TJIAN, R .
SCIENCE, 1987, 238 (4832) :1386-1392
[9]   EFFICIENT TRANSFORMATION OF CHICKEN-EMBRYO FIBROBLASTS BY C-JUN REQUIRES STRUCTURAL MODIFICATION IN CODING AND NONCODING SEQUENCES [J].
BOS, TJ ;
MONTECLARO, FS ;
MITSUNOBU, F ;
BALL, AR ;
CHANG, CHW ;
NISHIMURA, T ;
VOGT, PK .
GENES & DEVELOPMENT, 1990, 4 (10) :1677-1687
[10]   CHARACTERIZATION OF A MOUSE MULTIGENE FAMILY THAT ENCODES ZINC FINGER STRUCTURES [J].
CHAVRIER, P ;
LEMAIRE, P ;
REVELANT, O ;
BRAVO, R ;
CHARNAY, P .
MOLECULAR AND CELLULAR BIOLOGY, 1988, 8 (03) :1319-1326
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