ADENOVIRUS E1A PROTEINS CAN DISSOCIATE HETEROMERIC COMPLEXES INVOLVING THE E2F TRANSCRIPTION FACTOR - A NOVEL MECHANISM FOR E1A TRANSACTIVATION

被引：336

作者：

BAGCHI, S ^{[1
]}

RAYCHAUDHURI, P ^{[1
]}

NEVINS, JR ^{[1
]}

机构：

[1] DUKE UNIV, MED CTR, DEPT MICROBIOL & IMMUNOL, DURHAM, NC 27710 USA

来源：

CELL | 1990年 / 62卷 / 04期

关键词：

D O I：

10.1016/0092-8674(90)90112-R

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：

Adenovirus infection activates the E2F transcription factor, in part through the formation of a heteromeric protein complex involving a 19 kd E4 gene product that then allows cooperative and stable promoter binding. We now find that cellular factors are complexed to E2F in extracts of several uninfected cell lines. E1A proteins can dissociate these complexes, releasing free E2F. This activity of E1A is independent of conserved domain 3 but is dependent on conserved domain 2 sequence. The E1A-mediated dissociation of the complexes allows the E4 protein to interact with E2F, generating a stable DNA-protein complex with the E2 promoter and a stimulation of transcription. These experiments demonstrate a function for E1A in mediating a dissociation of transcription factor complexes, allowing new interactions to form and thus changing the transcriptional specificity. © 1990.

引用

页码：659 / 669

页数：11

共 61 条

[1] ACTIVATION OF DNA-BINDING ACTIVITY IN AN APPARENTLY CYTOPLASMIC PRECURSOR OF THE NF-KAPPA-B TRANSCRIPTION FACTOR [J].

BAEUERLE, PA ;

BALTIMORE, D .

CELL, 1988, 53 (02) :211-217

[2] PHOSPHORYLATION-DEPENDENT ACTIVATION OF THE ADENOVIRUS-INDUCIBLE E2F TRANSCRIPTION FACTOR IN A CELL-FREE SYSTEM [J].

BAGCHI, S ;

RAYCHAUDHURI, P ;

NEVINS, JR .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (12) :4352-4356

[3] DIFFERENTIAL ACTIVATION OF RNA POLYMERASE-III-TRANSCRIBED GENES BY THE POLYOMAVIRUS ENHANCER AND THE ADENOVIRUS E1A GENE-PRODUCTS [J].

BERGER, SL ;

FOLK, WR .

NUCLEIC ACIDS RESEARCH, 1985, 13 (04) :1413-1428

[4] ADENOVIRUS PROMOTERS AND E1A TRANSACTIVATION [J].

BERK, AJ .

ANNUAL REVIEW OF GENETICS, 1986, 20 :45-79

[5] SIZING AND MAPPING OF EARLY ADENOVIRUS MESSENGER-RNAS BY GEL-ELECTROPHORESIS OF S1 ENDONUCLEASE-DIGESTED HYBRIDS [J].

BERK, AJ ;

SHARP, PA .

CELL, 1977, 12 (03) :721-732

[6] TPA CAN OVERCOME THE REQUIREMENT FOR ELA AND TOGETHER ACT SYNERGISTICALLY IN STIMULATING EXPRESSION OF THE ADENOVIRUS-EIII PROMOTER [J].

BUCKBINDER, L ;

MIRALLES, VJ ;

REINBERG, D .

EMBO JOURNAL, 1989, 8 (13) :4239-4250

[7]

CULLEN BR, 1987, METHOD ENZYMOL, V152, P684

[8] SV40 LARGE TUMOR-ANTIGEN FORMS A SPECIFIC COMPLEX WITH THE PRODUCT OF THE RETINOBLASTOMA SUSCEPTIBILITY GENE [J].

DECAPRIO, JA ;

LUDLOW, JW ;

FIGGE, J ;

SHEW, JY ;

HUANG, CM ;

LEE, WH ;

MARSILIO, E ;

PAUCHA, E ;

LIVINGSTON, DM .

CELL, 1988, 54 (02) :275-283

[9] THE HUMAN PAPILLOMA VIRUS-16 E7-ONCOPROTEIN IS ABLE TO BIND TO THE RETINOBLASTOMA GENE-PRODUCT [J].

DYSON, N ;

HOWLEY, PM ;

MUNGER, K ;

HARLOW, E .

SCIENCE, 1989, 243 (4893) :934-937

[10] THE CELLULAR 107K-PROTEIN THAT BINDS TO ADENOVIRUS-E1A ALSO ASSOCIATES WITH THE LARGE T-ANTIGENS OF SV40 AND JC VIRUS [J].

DYSON, N ;

BUCHKOVICH, K ;

WHYTE, P ;

HARLOW, E .

CELL, 1989, 58 (02) :249-255

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