CALORIE RESTRICTION DELAYS SPONTANEOUS TUMORIGENESIS IN P53-KNOCKOUT TRANSGENIC MICE

被引：142

作者：

HURSTING, SD ^{[1
]}

PERKINS, SN ^{[1
]}

PHANG, JM ^{[1
]}

机构：

[1] NCI,FREDERICK CANC RES & DEV CTR,DIV CANC PREVENT & CONTROL,NUTR & MOLEC REGULAT LAB,FREDERICK,MD 21702

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1994年 / 91卷 / 15期

关键词：

D O I：

10.1073/pnas.91.15.7036

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：

Transgenic mice with both alleles of the p53 tumor suppressor gene (frequently mutated in human tumors) knocked out by gene targeting provide a potentially useful tumorigenesis model because these mice rapidly develop spontaneous tumors. To determine whether tumorigenesis in p53-knockout mice is sensitive to experimental manipulation, tumor development in response to calorie restriction (CR; a potent inhibitor of rodent tumors) was evaluated. Tumor development was monitored for 48 weeks in male nullizygous p53-knockout and wild-type littermate mice (28-30 per treatment group) fed ad libitum (AL) or restricted to 60% of AL carbohydrate calorie intake. CR:p53-knockout mice (median survival = 25 weeks) experienced a delay in tumor onset and subsequent mortality (P = 0.0002) relative to AL:p53-knockout mice (median survival = 16 weeks). Tumor development and mortality in wildtype littermates on either diet treatment were <4% through 48 weeks. Cell cycle analyses were performed on splenocytes from p53-knockout mice and wild-type littermates after 4 weeks of AL feeding or CR (5 per group). The percentage of splenocytes in S phase of the cell cycle was 3-fold higher for p53-knockout mice than wild-type mice (P < 0.001), and CR reduced the percentage of S-phase splenocytes in both p53-knockout and wild-type mice (P = 0.012). These data demonstrate that tumor development in p53-knockout mite genetically predisposed to tumors can be delayed by CR (possibly via cell cycle modulation) and suggest that these mice provide a very useful model of spontaneous tumorigenesis.

引用

页码：7036 / 7040

页数：5

共 21 条

[11] 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
[12] THE P53 TUMOR SUPPRESSOR GENE
LEVINE, AJ
MOMAND, J
FINLAY, CA
[J]. NATURE, 1991, 351 (6326) : 453 - 456
[13] LIVINGSTONE LR, 1992, CELL, V71, P587
[14] CALORIE RESTRICTION AND CELLULAR PROLIFERATION IN VARIOUS TISSUES OF THE FEMALE SWISS WEBSTER MOUSE
LOK, E
SCOTT, FW
MONGEAU, R
NERA, EA
MALCOLM, S
CLAYSON, DB
[J]. CANCER LETTERS, 1990, 51 (01) : 67 - 73
[15] TUMOR-SUPPRESSOR GENES - NO ROOM AT THE P53 INN
PIETENPOL, JA
[J]. NATURE, 1993, 365 (6441) : 17 - 18
[16] PURDIE CA, 1994, ONCOGENE, V9, P603
[17] GERM-LINE TRANSMISSION OF A MUTATED P53 GENE IN A CANCER-PRONE FAMILY WITH LI-FRAUMENI SYNDROME
SRIVASTAVA, S
ZOU, ZQ
PIROLLO, K
BLATTNER, W
CHANG, EH
[J]. NATURE, 1990, 348 (6303) : 747 - 749
[18] TREND AND HOMOGENEITY ANALYSES OF PROPORTIONS AND LIFE TABLE DATA
THOMAS, DG
BRESLOW, N
GART, JJ
[J]. COMPUTERS AND BIOMEDICAL RESEARCH, 1977, 10 (04): : 373 - 381
[19] PREPARATION OF TISSUES FOR DNA FLOW CYTOMETRIC ANALYSIS
THORNTHWAITE, JT
SUGARBAKER, EV
TEMPLE, WJ
[J]. CYTOMETRY, 1980, 1 (03): : 229 - 237
[20] WEINDRUCH R, 1988, RETARDATION AGING DI, P73

← 1 2 3 →