MICE LACKING P21(C/P1/WAF1) UNDERGO NORMAL DEVELOPMENT, BUT ARE DEFECTIVE IN G1 CHECKPOINT CONTROL

被引：1949

作者：

DENG, CX

ZHANG, PM

HARPER, JW

ELLEDGE, SJ

LEDER, P

机构：

[1] HARVARD UNIV,SCH MED,HOWARD HUGHES MED INST,BOSTON,MA 02115

[2] HARVARD UNIV,SCH MED,DEPT GENET,BOSTON,MA 02115

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

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

来源：

CELL | 1995年 / 82卷 / 04期

关键词：

D O I：

10.1016/0092-8674(95)90039-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：

p21(CIP1/WAF1) is a CDK inhibitor regulated by the tumor suppressor p53 and is hypothesized to mediate G1 arrest. p53 has been suggested to derive anti-oncogenic properties from this relationship. To test these notions, we created mice lacking p21(CIP1/WAF1). They develop normally and (unlike p53(-/-) mice) have not developed spontaneous malignancies during 7 months of observation. Nonetheless, p21(-/-) embryonic fibroblasts are significantly deficient in their ability to arrest in G1 in response to DNA damage and nucleotide pool perturbation. p21(-/-) cells also exhibit a significant growth alteration in vitro, achieving a saturation density as high as that observed In p53(-/-) cells. In contrast, other aspects of p53 function, such as thymocytic apoptosis and the mitotic spindle checkpoint, appear normal. These results establish the role of p21(CIP1/WAF1) in the G1 checkpoint, but suggest that the anti-apoptotic and the anti-oncogenic effects of p53 are more complex.

引用

页码：675 / 684

页数：10

共 64 条

[31] WILD-TYPE P53 IS A CELL-CYCLE CHECKPOINT DETERMINANT FOLLOWING IRRADIATION
KUERBITZ, SJ
PLUNKETT, BS
WALSH, WV
KASTAN, MB
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (16) : 7491 - 7495
[32] CLONING OR P57(KIP2), A CYCLIN-DEPENDENT KINASE INHIBITOR WITH UNIQUE DOMAIN-STRUCTURE AND TISSUE DISTRIBUTION
LEE, MH
REYNISDOTTIR, I
MASSAGUE, J
[J]. GENES & DEVELOPMENT, 1995, 9 (06) : 639 - 649
[33] ALTERED CELL-CYCLE ARREST AND GENE AMPLIFICATION POTENTIAL ACCOMPANY LOSS OF WILD-TYPE P53
LIVINGSTONE, LR
WHITE, A
SPROUSE, J
LIVANOS, E
JACKS, T
TISTY, TD
[J]. CELL, 1992, 70 (06) : 923 - 935
[34] HEMATOPOIETIC-CELLS FROM MICE DEFICIENT IN WILD-TYPE P53 ARE MORE RESISTANT TO INDUCTION OF APOPTOSIS BY SOME AGENTS
LOTEM, J
SACHS, L
[J]. BLOOD, 1993, 82 (04) : 1092 - 1096
[35] P53 IS REQUIRED FOR RADIATION-INDUCED APOPTOSIS IN MOUSE THYMOCYTES
LOWE, SW
SCHMITT, EM
SMITH, SW
OSBORNE, BA
JACKS, T
[J]. NATURE, 1993, 362 (6423) : 847 - 849
[36] P53-DEPENDENT AND INDEPENDENT EXPRESSION OF P21 DURING CELL-GROWTH, DIFFERENTIATION, AND DNA-DAMAGE
MACLEOD, KF
SHERRY, N
HANNON, G
BEACH, D
TOKINO, T
KINZLER, K
VOGELSTEIN, B
JACKS, T
[J]. GENES & DEVELOPMENT, 1995, 9 (08) : 935 - 944
[37] UV IRRADIATION STIMULATES LEVELS OF P53 CELLULAR TUMOR-ANTIGEN IN NONTRANSFORMED MOUSE CELLS
MALTZMAN, W
CZYZYK, L
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1984, 4 (09) : 1689 - 1694
[38] P57(KIP2), A STRUCTURALLY DISTINCT MEMBER OF THE P21(CIP1) CDK INHIBITOR FAMILY, IS A CANDIDATE TUMOR-SUPPRESSOR GENE
MATSUOKA, S
EDWARDS, MC
BAI, C
PARKER, S
ZHANG, PM
BALDINI, A
HARPER, JW
ELLEDGE, SJ
[J]. GENES & DEVELOPMENT, 1995, 9 (06) : 650 - 662
[39] MIYASHITA T, 1995, CELL, V80, P293
[40] CLONING OF SENESCENT CELL-DERIVED INHIBITORS OF DNA-SYNTHESIS USING AN EXPRESSION SCREEN
NODA, A
NING, Y
VENABLE, SF
PEREIRASMITH, OM
SMITH, JR
[J]. EXPERIMENTAL CELL RESEARCH, 1994, 211 (01) : 90 - 98

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