SEQUENCE-SPECIFIC TRANSCRIPTIONAL ACTIVATION IS ESSENTIAL FOR GROWTH SUPPRESSION BY P53

被引：413

作者：

PIETENPOL, JA

TOKINO, T

THIAGALINGAM, S

ELDEIRY, WS

KINZLER, KW

VOGELSTEIN, B

机构：

[1] Oncology Center, Johns Hopkins University, School of Medicine, Baltimore, MD 21231

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1994年 / 91卷 / 06期

关键词：

D O I：

10.1073/pnas.91.6.1998

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Although several biochemical features of p53 have been described, their relationship to tumor suppression remains uncertain. We have compared the ability of p53-derived proteins to act as sequence-specific transcriptional (SST) activators with their ability to suppress tumor cell growth, using an improved growth-suppression assay. Both naturally occurring and in vitro derived mutations that abrogated the SST activity of p53 lost the ability to suppress tumor cell growth. Additionally, the N- and C-terminal ends of p53 were shown to be functionally replaceable with foreign transactivation and dimerization domains, respectively, with concordant preservation of both SST and tumor-suppressive properties. Only the central region of p53, conferring specific DNA binding, was required to suppress growth by such hybrid proteins. The SST activity of p53 thus appeared to be essential for the protein to function as a tumor suppressor.

引用

页码：1998 / 2002

页数：5

共 32 条

[1] OVERLAP OF THE P53-RESPONSIVE ELEMENT AND CAMP-RESPONSIVE ELEMENT IN THE ENHANCER OF HUMAN T-CELL LEUKEMIA-VIRUS TYPE-I
AOYAMA, N
NAGASE, T
SAWAZAKI, T
MIZUGUCHI, G
NAKAGOSHI, H
FUJISAWA, JI
YOSHIDA, M
ISHII, S
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (12) : 5403 - 5407
[2] SUPPRESSION OF HUMAN COLORECTAL-CARCINOMA CELL-GROWTH BY WILD-TYPE-P53
BAKER, SJ
MARKOWITZ, S
FEARON, ER
WILLSON, JKV
VOGELSTEIN, B
[J]. SCIENCE, 1990, 249 (4971) : 912 - 915
[3] CONNECTIONS BETWEEN TRANSCRIPTIONAL ACTIVATORS, SILENCERS, AND TELOMERES AS REVEALED BY FUNCTIONAL-ANALYSIS OF A YEAST DNA-BINDING PROTEIN
BUCHMAN, AR
LUE, NF
KORNBERG, RD
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1988, 8 (12) : 5086 - 5099
[4] CHEN JY, 1993, ONCOGENE, V8, P2159
[5] MICE DEFICIENT FOR P53 ARE DEVELOPMENTALLY NORMAL BUT SUSCEPTIBLE TO SPONTANEOUS TUMORS
DONEHOWER, LA
HARVEY, M
SLAGLE, BL
MCARTHUR, MJ
MONTGOMERY, CA
BUTEL, JS
BRADLEY, A
[J]. NATURE, 1992, 356 (6366) : 215 - 221
[6] DEFINITION OF A CONSENSUS BINDING-SITE FOR P53
ELDEIRY, WS
KERN, SE
PIETENPOL, JA
KINZLER, KW
VOGELSTEIN, B
[J]. NATURE GENETICS, 1992, 1 (01) : 45 - 49
[7] WAF1, A POTENTIAL MEDIATOR OF P53 TUMOR SUPPRESSION
ELDEIRY, WS
TOKINO, T
VELCULESCU, VE
LEVY, DB
PARSONS, R
TRENT, JM
LIN, D
MERCER, WE
KINZLER, KW
VOGELSTEIN, B
[J]. CELL, 1993, 75 (04) : 817 - 825
[8] THE GCN4 BASIC REGION LEUCINE ZIPPER BINDS DNA AS A DIMER OF UNINTERRUPTED ALPHA-HELICES - CRYSTAL-STRUCTURE OF THE PROTEIN-DNA COMPLEX
ELLENBERGER, TE
BRANDL, CJ
STRUHL, K
HARRISON, SC
[J]. CELL, 1992, 71 (07) : 1223 - 1237
[9] PRESENCE OF A POTENT TRANSCRIPTION ACTIVATING SEQUENCE IN THE P53 PROTEIN
FIELDS, S
JANG, SK
[J]. SCIENCE, 1990, 249 (4972) : 1046 - 1049
[10] A TRANSCRIPTIONALLY ACTIVE DNA-BINDING SITE FOR HUMAN P53 PROTEIN COMPLEXES
FUNK, WD
PAK, DT
KARAS, RH
WRIGHT, WE
SHAY, JW
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1992, 12 (06) : 2866 - 2871

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