GADD45b and GADD45g are cdc2/cyclinB1 kinase inhibitors with a role in S and G2/M cell cycle checkpoints induced by genotoxic stress

被引：288

作者：

Vairapandi, M

Balliet, AG

Hoffman, B

Liebermann, DA

机构：

[1] Temple Univ, Sch Med, Fels Inst Canc Res & Mol Biol, Philadelphia, PA 19140 USA

[2] Temple Univ, Sch Med, Dept Biochem, Philadelphia, PA 19140 USA

来源：

JOURNAL OF CELLULAR PHYSIOLOGY | 2002年 / 192卷 / 03期

关键词：

D O I：

10.1002/jcp.10140

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Gadd45a (Gadd45), Gadd45b (MyD118), and Gadd45g (CR6) constitute a family of evolutionarily conserved, small, acidic, nuclear proteins, which have been implicated in terminal differentiation, growth suppression, and apoptosis. How Gadd45 proteins function in negative growth control is not fully understood. Recent evidence has implicated Gadd45a in inhibition of cdc2/cyclinB1 kinase and in G2/M cell cycle arrest. Yet, whether Gadd45b and/or Gadd45g function as inhibitors of cdc2/cyclinB1 kinase and/or play a role in G2/M cell cycle arrest has not been fully established. In this work, we show that Gadd45b and Gadd45g specifically interact with the Cdk1/CyclinB1 complex, but not with other Cdk/Cyclin complexes, in vitro and in vivo. Data also has been obtained that Gadd45b and Gadd45g, as well as GADD45a, interact with both Cdk1 and cyclinB1, resulting in inhibition of the kinase activity of the Cdk1/cyclinB1 complex. Inhibition of Cdk1/cyclinB1 kinase activity by Gadd45b and Gadd45a was found to involve disruption of the complex, whereas Gadd45g did not disrupt the complex. Moreover, using RKO lung carcinoma cell lines, which express antisense Gadd45 RNA, data has been obtained, which indicates that all three Gadd45 proteins are likely to cooperate in activation of S and G2/M checkpoints following exposure of cells to UV irradiation. (C) 2002 Wiley-Liss, Inc.

引用

页码：327 / 338

页数：12

共 37 条

[1] ABDOLLAHI A, 1991, ONCOGENE, V6, P165
[2] Interaction of CR6 (GADD45γ) with proliferating cell nuclear antigen impedes negative growth control
Azam, N
Vairapandi, M
Zhang, W
Hoffman, B
Liebermann, DA
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 2001, 276 (04) : 2766 - 2774
[3] ISOLATION OF INTERLEUKIN-2-INDUCED IMMEDIATE-EARLY GENES
BEADLING, C
JOHNSON, KW
SMITH, KA
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (07) : 2719 - 2723
[4] Chan TA, 2000, GENE DEV, V14, P1584
[5] MICE LACKING P21(C/P1/WAF1) UNDERGO NORMAL DEVELOPMENT, BUT ARE DEFECTIVE IN G1 CHECKPOINT CONTROL
DENG, CX
ZHANG, PM
HARPER, JW
ELLEDGE, SJ
LEDER, P
[J]. CELL, 1995, 82 (04) : 675 - 684
[6] 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
[7] Cell cycle checkpoints: Preventing an identity crisis
Elledge, SJ
[J]. SCIENCE, 1996, 274 (5293) : 1664 - 1672
[8] MAMMALIAN GENES COORDINATELY REGULATED BY GROWTH ARREST SIGNALS AND DNA-DAMAGING AGENTS
FORNACE, AJ
NEBERT, DW
HOLLANDER, MC
LUETHY, JD
PAPATHANASIOU, M
FARGNOLI, J
HOLBROOK, NJ
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1989, 9 (10) : 4196 - 4203
[9] GENOTOXIC-STRESS-RESPONSE GENES AND GROWTH-ARREST GENES - GADD, MYD, AND OTHER GENES INDUCED BY TREATMENTS ELICITING GROWTH ARREST
FORNACE, AJ
JACKMAN, J
HOLLANDER, MC
HOFFMANLIEBERMANN, B
LIEBERMANN, DA
[J]. ANNALS OF THE NEW YORK ACADEMY OF SCIENCES-SERIES, 1992, 663 : 139 - 153
[10] FORNACE AJ, 1992, ANNU REV GENET, V26, P507

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