P57(KIP2), A STRUCTURALLY DISTINCT MEMBER OF THE P21(CIP1) CDK INHIBITOR FAMILY, IS A CANDIDATE TUMOR-SUPPRESSOR GENE

被引：917

作者：

MATSUOKA, S

EDWARDS, MC

BAI, C

PARKER, S

ZHANG, PM

BALDINI, A

HARPER, JW

ELLEDGE, SJ

机构：

[1] BAYLOR COLL MED,HOWARD HUGHES MED INST,HOUSTON,TX 77030

[2] BAYLOR COLL MED,VERNA & MARRS MCLEAN DEPT BIOCHEM,HOUSTON,TX 77030

[3] BAYLOR COLL MED,DEPT HUMAN & MOLEC GENET,HOUSTON,TX 77030

来源：

GENES & DEVELOPMENT | 1995年 / 9卷 / 06期

关键词：

P57(KIP2); P21(CIP1); CDK INHIBITOR; TUMOR SUPPRESSOR; CELL CYCLE;

D O I：

10.1101/gad.9.6.650

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Cydin-dependent kinases (Cdks) are positive regulators of cell proliferation, whereas Cdk inhibitors (CKIs) inhibit proliferation. We describe a new CKI, p57(KIP2), which is related to p21(CIP1) and p27(KIP1). p57(KIP2) is a potent, tight-binding inhibitor of several G(1) cyclin/Cdk complexes, and its binding is cyclin dependent. Unlike CIP1, KIP2 is not regulated by p53. Overexpression of p57(KIP2) arrests cells in G(1). p57(KIP2) proteins have a complex structure. Mouse p57(KIP2) consists Of four structurally distinct domains: an amino-terminal Cdk inhibitory domain, a proline-rich domain, an acidic-repeat region, and a carboxy-terminal domain conserved with p27(KIP1). Human p57(KIP2) appears to have conserved the amino- and carboxy-terminal domains but has replaced the internal regions with sequences containing proline-alanine repeats. In situ hybridization during mouse embryogenesis revealed that KIP2 mRNA displays a striking pattern of expression during development, showing high level expression in skeletal muscle, brain, heart, lungs, and eye. Most of the KIP2-expressing cells are terminally differentiated, suggesting that p57(KIP2) is involved in decisions to exit the cell cycle during development and differentiation. Human KIP2 is located at 11p15.5, a region implicated in both sporadic cancers and Beckwith-Wiedemann syndrome, a familial cancer syndrome, marking it as a candidate tumor suppressor. The discovery of a new member of the p21(CIP1) inhibitor family with novel structural features and expression patterns suggests a complex role for these proteins in cell cycle control and development.

引用

页码：650 / 662

页数：13

共 50 条

[1] HUMAN CYCLIN-F
BAI, C
RICHMAN, R
ELLEDGE, SJ
[J]. EMBO JOURNAL, 1994, 13 (24) : 6087 - 6098
[2] RATES OF P16(MTS1) MUTATIONS IN PRIMARY TUMORS WITH 9P LOSS
CAIRNS, P
MAO, L
MERLO, A
LEE, DJ
SCHWAB, D
EBY, Y
TOKINO, K
VANDERRIET, P
BLAUGRUND, JE
SIDRANSKY, D
[J]. SCIENCE, 1994, 265 (5170) : 415 - 416
[3] Draetta Giulio, 1993, Trends in Cell Biology, V3, P287, DOI 10.1016/0962-8924(93)90001-H
[4] P53-DEPENDENT INHIBITION OF CYCLIN-DEPENDENT KINASE-ACTIVITIES IN HUMAN FIBROBLASTS DURING RADIATION-INDUCED G1 ARREST
DULIC, V
KAUFMANN, WK
WILSON, SJ
TLSTY, TD
LEES, E
HARPER, JW
ELLEDGE, SJ
REED, SI
[J]. CELL, 1994, 76 (06) : 1013 - 1023
[5] THE RETINOBLASTOMA PROTEIN ASSOCIATES WITH THE PROTEIN PHOSPHATASE TYPE-1 CATALYTIC SUBUNIT
DURFEE, T
BECHERER, K
CHEN, PL
YEH, SH
YANG, YZ
KILBURN, AE
LEE, WH
ELLEDGE, SJ
[J]. GENES & DEVELOPMENT, 1993, 7 (04) : 555 - 569
[6] ELDEIRY WS, 1994, CANCER RES, V54, P1169
[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] CDK2 ENCODES A 33-KDA CYCLIN-A-ASSOCIATED PROTEIN-KINASE AND IS EXPRESSED BEFORE CDC2 IN THE CELL-CYCLE
ELLEDGE, SJ
RICHMAN, R
HALL, FL
WILLIAMS, RT
LODGSON, N
HARPER, JW
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (07) : 2907 - 2911
[9] 2 GENES DIFFERENTIALLY REGULATED IN THE CELL-CYCLE AND BY DNA-DAMAGING AGENTS ENCODE ALTERNATIVE REGULATORY SUBUNITS OF RIBONUCLEOTIDE REDUCTASE
ELLEDGE, SJ
DAVIS, RW
[J]. GENES & DEVELOPMENT, 1990, 4 (05) : 740 - 751
[10] ELLEDGE SJ, 1994, CURR OPIN CELL BIOL, V6, P874

← 1 2 3 4 5 →