Inhibition of E2F-mediated transcription by p202

被引：100

作者：

Choubey, D ^{[1
]}

Li, SJ ^{[1
]}

Datta, B ^{[1
]}

Gutterman, JU ^{[1
]}

Lengyel, P ^{[1
]}

机构：

[1] YALE UNIV,DEPT BIOCHEM & MOL BIOPHYS,NEW HAVEN,CT 06520

来源：

EMBO JOURNAL | 1996年 / 15卷 / 20期

关键词：

cell growth inhibition; E3F binding protein; inhibition of E2F-mediated transcription; interferon-inducible p202;

D O I：

10.1002/j.1460-2075.1996.tb00951.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：

Many of the antimicrobial, immunomodulatory and cell growth inhibitory activities of the interferons are mediated by interferon-inducible proteins. Earlier we characterized an interferon-inducible murine protein, p202, whose expression in transfected cells inhibits cell proliferation and which can form a complex,vith retinoblastoma protein (pRb). Here we report that in transfected cells expression of p202 inhibits E2F-stimulated transcription of a reporter gene and of endogenous genes. Inhibition of the transcriptional activity of E2F by p202 does not depend on fully functional pRb and is correlated with inhibition of the sequence-specific DNA binding of E2F. p202 interacts with the transcription factor E2F (E2F-1/DP-1) in vitro and in vivo. Inhibition of E2F activity by p202 may contribute to growth inhibition by the interferons.

引用

页码：5668 / 5678

页数：11

共 69 条

[1] TRANSCRIPTIONAL CONTROL BY E2F [J].

ADAMS, PD ;

KAELIN, WG .

SEMINARS IN CANCER BIOLOGY, 1995, 6 (02) :99-108

[2] ADENOVIRUS E1A PROTEINS CAN DISSOCIATE HETEROMERIC COMPLEXES INVOLVING THE E2F TRANSCRIPTION FACTOR - A NOVEL MECHANISM FOR E1A TRANSACTIVATION [J].

BAGCHI, S ;

RAYCHAUDHURI, P ;

NEVINS, JR .

CELL, 1990, 62 (04) :659-669

[3] THE RETINOBLASTOMA PROTEIN COPURIFIES WITH E2F-I, AN E1A-REGULATED INHIBITOR OF THE TRANSCRIPTION FACTOR E2F [J].

BAGCHI, S ;

WEINMANN, R ;

RAYCHAUDHURI, P .

CELL, 1991, 65 (06) :1063-1072

[4] FUNCTIONAL SYNERGY BETWEEN DP-1 AND E2F-1 IN THE CELL CYCLE-REGULATING TRANSCRIPTION FACTOR DRTF1/E2F [J].

BANDARA, LR ;

BUCK, VM ;

ZAMANIAN, M ;

JOHNSTON, LH ;

LATHANGUE, NB .

EMBO JOURNAL, 1993, 12 (11) :4317-4324

[5] ADENOVIRUS-E1A PREVENTS THE RETINOBLASTOMA GENE-PRODUCT FROM COMPLEXING WITH A CELLULAR TRANSCRIPTION FACTOR [J].

BANDARA, LR ;

LATHANGUE, NB .

NATURE, 1991, 351 (6326) :494-497

[6] REGULATION OF THE RETINOBLASTOMA PROTEIN-RELATED P107 BY G(1) CYCLIN COMPLEXES [J].

BEIJERSBERGEN, RL ;

CARLEE, L ;

KERKHOVEN, RM ;

BERNARDS, R .

GENES & DEVELOPMENT, 1995, 9 (11) :1340-1353

[7] E2F-4, A NEW MEMBER OF THE E2F GENE FAMILY, HAS ONCOGENIC ACTIVITY AND ASSOCIATES WITH P107 IN-VIVO [J].

BEIJERSBERGEN, RL ;

KERKHOVEN, RM ;

ZHU, LA ;

CARLEE, L ;

VOORHOEVE, PM ;

BERNARDS, R .

GENES & DEVELOPMENT, 1994, 8 (22) :2680-2690

[8] TRANSCRIPTION FACTOR E2F IS REQUIRED FOR EFFICIENT EXPRESSION OF THE HAMSTER DIHYDROFOLATE-REDUCTASE GENE INVITRO AND INVIVO [J].

BLAKE, MC ;

AZIZKHAN, JC .

MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (11) :4994-5002

[9] THE E2F TRANSCRIPTION FACTOR IS A CELLULAR TARGET FOR THE RB PROTEIN [J].

CHELLAPPAN, SP ;

HIEBERT, S ;

MUDRYJ, M ;

HOROWITZ, JM ;

NEVINS, JR .

CELL, 1991, 65 (06) :1053-1061

[10] THE T/E1A-BINDING DOMAIN OF THE RETINOBLASTOMA PRODUCT CAN INTERACT SELECTIVELY WITH A SEQUENCE-SPECIFIC DNA-BINDING PROTEIN [J].

CHITTENDEN, T ;

LIVINGSTON, DM ;

KAELIN, WG .

CELL, 1991, 65 (06) :1073-1082

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