WILD-TYPE ALTERNATIVELY SPLICED P53 - BINDING TO DNA AND INTERACTION WITH THE MAJOR P53 PROTEIN IN-VITRO AND IN CELLS

被引：55

作者：

WU, Y ^{[1
]}

LIU, YG ^{[1
]}

LEE, L ^{[1
]}

MINER, Z ^{[1
]}

KULESZMARTIN, M ^{[1
]}

机构：

[1] ROSWELL PK CANC INST, DEPT EXPTL THERAPEUT, BUFFALO, NY 14263 USA

来源：

EMBO JOURNAL | 1994年 / 13卷 / 20期

关键词：

ALTERNATIVE SPLICING; DNA BINDING; WILD-TYPE P53 PROTEIN;

D O I：

10.1002/j.1460-2075.1994.tb06808.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：

A p53 variant protein (p53as) generated from alternatively spliced p53 RNA is expressed in normal and malignant mouse cells and tissues, and p53as antigen activity is preferentially associated with the Gz phase of the cell cycle, suggesting that p53as and p53 protein may have distinct properties. Using p53as and p53 proteins translated bl vitro, we now provide evidence that p53as protein has efficient sequence-specific DNA-binding ability. DNA binding by p53 protein is inefficient in comparison and requires activation. Furthermore, p53as and p53 proteins formed hetero-oligomers when co-translated in vitro, resulting in inactivation of p53as DNA-binding activity. Gel filtration indicated that p53as translated in vitro, like p53, formed tetramers. In support of a functional role of p53as in cells, p53as/p53 hetero-oligomers were coimmunoprecipitated from mouse cells, and both protein forms were detectable in nuclear extracts by electrophoretic mobility shift assays. These results suggest that the biochemical functions of p53 are mediated by interaction between two endogenous protein products of the wild-type p53 gene.

引用

页码：4823 / 4830

页数：8

共 38 条

[1] IMMUNOLOGICALLY DISTINCT P53 MOLECULES GENERATED BY ALTERNATIVE SPLICING [J].

ARAI, N ;

NOMURA, D ;

YOKOTA, K ;

WOLF, D ;

BRILL, E ;

SHOHAT, O ;

ROTTER, V .

MOLECULAR AND CELLULAR BIOLOGY, 1986, 6 (09) :3232-3239

[2] MDM2 EXPRESSION IS INDUCED BY WILD TYPE-P53 ACTIVITY [J].

BARAK, Y ;

JUVEN, T ;

HAFFNER, R ;

OREN, M .

EMBO JOURNAL, 1993, 12 (02) :461-468

[3] A PROTEOLYTIC FRAGMENT FROM THE CENTRAL REGION OF P53 HAS MARKED SEQUENCE-SPECIFIC DNA-BINDING ACTIVITY WHEN GENERATED FROM WILD-TYPE BUT NOT FROM ONCOGENIC MUTANT P53-PROTEIN [J].

BARGONETTI, J ;

MANFREDI, JJ ;

CHEN, XB ;

MARSHAK, DR ;

PRIVES, C .

GENES & DEVELOPMENT, 1993, 7 (12B) :2565-2574

[4] WILD-TYPE BUT NOT MUTANT P53 IMMUNOPURIFIED PROTEINS BIND TO SEQUENCES ADJACENT TO THE SV40 ORIGIN OF REPLICATION [J].

BARGONETTI, J ;

FRIEDMAN, PN ;

KERN, SE ;

VOGELSTEIN, B ;

PRIVES, C .

CELL, 1991, 65 (06) :1083-1091

[5] DEFINITION OF A CONSENSUS BINDING-SITE FOR P53 [J].

ELDEIRY, WS ;

KERN, SE ;

PIETENPOL, JA ;

KINZLER, KW ;

VOGELSTEIN, B .

NATURE GENETICS, 1992, 1 (01) :45-49

[6] WAF1, A POTENTIAL MEDIATOR OF P53 TUMOR SUPPRESSION [J].

ELDEIRY, WS ;

TOKINO, T ;

VELCULESCU, VE ;

LEVY, DB ;

PARSONS, R ;

TRENT, JM ;

LIN, D ;

MERCER, WE ;

KINZLER, KW ;

VOGELSTEIN, B .

CELL, 1993, 75 (04) :817-825

[7] WILD-TYPE P53 ACTIVATES TRANSCRIPTION INVITRO [J].

FARMER, G ;

BARGONETTI, J ;

ZHU, H ;

FRIEDMAN, P ;

PRYWES, R ;

PRIVES, C .

NATURE, 1992, 358 (6381) :83-86

[8] THE MDM-2 ONCOGENE CAN OVERCOME WILD-TYPE P53 SUPPRESSION OF TRANSFORMED-CELL GROWTH [J].

FINLAY, CA .

MOLECULAR AND CELLULAR BIOLOGY, 1993, 13 (01) :301-306

[9] THE P53 PROTEIN IS AN UNUSUALLY SHAPED TETRAMER THAT BINDS DIRECTLY TO DNA [J].

FRIEDMAN, PN ;

CHEN, XB ;

BARGONETTI, J ;

PRIVES, C .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (08) :3319-3323

[10] A TRANSCRIPTIONALLY ACTIVE DNA-BINDING SITE FOR HUMAN P53 PROTEIN COMPLEXES [J].

FUNK, WD ;

PAK, DT ;

KARAS, RH ;

WRIGHT, WE ;

SHAY, JW .

MOLECULAR AND CELLULAR BIOLOGY, 1992, 12 (06) :2866-2871

← 1 2 3 4 →