Signalling to p53: Where does it all start?

被引：35

作者：

Kastan, MB

机构：

[1] Johns Hopkins University, Baltimore, MD 21205, 720 Rutland Avenue

来源：

BIOESSAYS | 1996年 / 18卷 / 08期

关键词：

D O I：

10.1002/bies.950180804

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：

Alterations in the p53 gene product appear to be a major factor in human tumorigenesis and may influence the responses of many human tumors to therapy. Much effort has focused on understanding the signals which normally initiate p53 growth-suppressive functions. Though it has been known that DNA damage can induce p53, a recent publication reports data which suggest that p53 can be induced by depletion of ribonucleotide pools, even in the absence of detectable DNA damage((1)). These observations provide new ideas about how cells utilize the p53 signal and open up new avenues of investigation for manipulating p53 function.

引用

收藏

页码：617 / 619

页数：3

相关论文

共 28 条

[1] P53 BINDS SINGLE-STRANDED-DNA ENDS THROUGH THE C-TERMINAL DOMAIN AND INTERNAL DNA SEGMENTS VIA THE MIDDLE DOMAIN [J].

BAKALKIN, G ;

SELIVANOVA, G ;

YAKOVLEVA, T ;

KISELEVA, E ;

KASHUBA, E ;

MAGNUSSON, KP ;

SZEKELY, L ;

KLEIN, G ;

TERENIUS, L ;

WIMAN, KG .

NUCLEIC ACIDS RESEARCH, 1995, 23 (03) :362-369

[2] P53 BINDS SINGLE-STRANDED-DNA ENDS AND CATALYZES DNA RENATURATION AND STRAND TRANSFER [J].

BAKALKIN, G ;

YAKOVLEVA, T ;

SELIVANOVA, G ;

MAGNUSSON, KP ;

SZEKELY, L ;

KISELEVA, E ;

KLEIN, G ;

TERENIUS, L ;

WIMAN, KG .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (01) :413-417

[3] SUPPRESSION OF HUMAN COLORECTAL-CARCINOMA CELL-GROWTH BY WILD-TYPE-P53 [J].

BAKER, SJ ;

MARKOWITZ, S ;

FEARON, ER ;

WILLSON, JKV ;

VOGELSTEIN, B .

SCIENCE, 1990, 249 (4971) :912-915

[4] THYMOCYTE APOPTOSIS INDUCED BY P53-DEPENDENT AND INDEPENDENT PATHWAYS [J].

CLARKE, AR ;

PURDIE, CA ;

HARRISON, DJ ;

MORRIS, RG ;

BIRD, CC ;

HOOPER, ML ;

WYLLIE, AH .

NATURE, 1993, 362 (6423) :849-852

[5] P53 FUNCTIONS AS A CELL-CYCLE CONTROL PROTEIN IN OSTEOSARCOMAS [J].

DILLER, L ;

KASSEL, J ;

NELSON, CE ;

GRYKA, MA ;

LITWAK, G ;

GEBHARDT, M ;

BRESSAC, B ;

OZTURK, M ;

BAKER, SJ ;

VOGELSTEIN, B ;

FRIEND, SH .

MOLECULAR AND CELLULAR BIOLOGY, 1990, 10 (11) :5772-5781

[6] MICE DEFICIENT FOR P53 ARE DEVELOPMENTALLY NORMAL BUT SUSCEPTIBLE TO SPONTANEOUS TUMORS [J].

DONEHOWER, LA ;

HARVEY, M ;

SLAGLE, BL ;

MCARTHUR, MJ ;

MONTGOMERY, CA ;

BUTEL, JS ;

BRADLEY, A .

NATURE, 1992, 356 (6366) :215-221

[7] DEFICIENCY OF P53 ACCELERATES MAMMARY TUMORIGENESIS IN WNT-1 TRANSGENIC MICE AND PROMOTES CHROMOSOMAL INSTABILITY [J].

DONEHOWER, LA ;

GODLEY, LA ;

ALDAZ, CM ;

PYLE, R ;

SHI, YP ;

PINKEL, D ;

GRAY, T ;

BRADLEY, A ;

MEDINA, D ;

VARMUS, HE .

GENES & DEVELOPMENT, 1995, 9 (07) :882-895

[8] PARTICIPATION OF P53 CELLULAR TUMOR-ANTIGEN IN TRANSFORMATION OF NORMAL EMBRYONIC-CELLS [J].

ELIYAHU, D ;

RAZ, A ;

GRUSS, P ;

GIVOL, D ;

OREN, M .

NATURE, 1984, 312 (5995) :646-649

[9] Hypoxia-mediated selection of cells with diminished apoptotic potential in solid tumours [J].

Graeber, TG ;

Osmanian, C ;

Jacks, T ;

Housman, DE ;

Koch, CJ ;

Lowe, SW ;

Giaccia, AJ .

NATURE, 1996, 379 (6560) :88-91

[10] HYPOXIA INDUCES ACCUMULATION OF P53 PROTEIN, BUT ACTIVATION OF A G(1)-PHASE CHECKPOINT BY LOW-OXYGEN CONDITIONS IS INDEPENDENT OF P53 STATUS [J].

GRAEBER, TG ;

PETERSON, JF ;

TSAI, M ;

MONICA, K ;

FORNACE, AJ ;

GIACCIA, AJ .

MOLECULAR AND CELLULAR BIOLOGY, 1994, 14 (09) :6264-6277