p53 Mutations in Human Cancers
Abstract
Mutations in the evolutionarily conserved codons of the p53 tumor suppressor gene are common in diverse types of human cancer. The p53 mutational spectrum differs among cancers of the colon, lung, esophagus, breast, liver, brain, reticuloendothelial tissues, and hemopoietic tissues. Analysis of these mutations can provide clues to the etiology of these diverse tumors and to the function of specific regions of p53. Transitions predominate in colon, brain, and lymphoid malignancies, whereas G:C to T:A transversions are the most frequent substitutions observed in cancers of the lung and liver. Mutations at A:T base pairs are seen more frequently in esophageal carcinomas than in other solid tumors. Most transitions in colorectal carcinomas, brain tumors, leukemias, and lymphomas are at CpG dinucleotide mutational hot spots. G to T transversions in lung, breast, and esophageal carcinomas are dispersed among numerous codons. In liver tumors in persons from geographic areas in which both aflatoxin B1 and hepatitis B virus are cancer risk factors, most mutations are at one nucleotide pair of codon 249. These differences may reflect the etiological contributions of both exogenous and endogenous factors to human carcinogenesis.
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References
IARC Monographs on the Evaluation of Carcinogenic Risks to Humans: Overall Evaluations of Carcinogenicity: An Updating of IARC Monographs Volumes 1 to 42 1 (1987).
World Health Organization, Cancer: Causes, Occurrence and Control (1990).
ADELMAN, R, OXIDATIVE DAMAGE TO DNA - RELATION TO SPECIES METABOLIC-RATE AND LIFE-SPAN, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 85: 2706 (1988).
AHUJA, H, ALTERATIONS IN THE P53 GENE AND THE CLONAL EVOLUTION OF THE BLAST CRISIS OF CHRONIC MYELOCYTIC-LEUKEMIA, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 86: 6783 (1989).
AMES, B.N., CHEMICAL CARCINOGENESIS - TOO MANY RODENT CARCINOGENS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 7772 (1990).
BAKER, S.J., P53 GENE-MUTATIONS OCCUR IN COMBINATION WITH 17P ALLELIC DELETIONS AS LATE EVENTS IN COLORECTAL TUMORIGENESIS, CANCER RESEARCH 50: 7717 (1990).
BAKER, S.J., CHROMOSOME-17 DELETIONS AND P53 GENE-MUTATIONS IN COLORECTAL CARCINOMAS, SCIENCE 244: 217 (1989).
BAKER, S.J., SUPPRESSION OF HUMAN COLORECTAL-CARCINOMA CELL-GROWTH BY WILD-TYPE-P53, SCIENCE 249: 912 (1990).
BALMAIN, A, ONCOGENE ACTIVATION IN CHEMICAL CARCINOGENESIS, ADVANCES IN CANCER RESEARCH 51: 147 (1988).
BARBACID, M, RAS GENES, ANNUAL REVIEW OF BIOCHEMISTRY 56: 779 (1987).
BARTEK, J, GENETIC AND IMMUNOCHEMICAL ANALYSIS OF MUTANT P53 IN HUMAN BREAST-CANCER CELL-LINES, ONCOGENE 5: 893 (1990).
Bennett, W., Oncogene 6: 1779 (1991).
BOHR, V.A., HETEROGENEOUS DNA DAMAGE AND REPAIR IN THE MAMMALIAN GENOME, CANCER RESEARCH 47: 6426 (1987).
BREIMER, L.H., MOLECULAR MECHANISMS OF OXYGEN RADICAL CARCINOGENESIS AND MUTAGENESIS - THE ROLE OF DNA-BASE DAMAGE, MOLECULAR CARCINOGENESIS 3: 188 (1990).
BRESSAC, B, SELECTIVE G-MUTATION TO T-MUTATION OF P53 GENE IN HEPATOCELLULAR-CARCINOMA FROM SOUTHERN AFRICA, NATURE 350: 429 (1991).
BRESSAC, B, ABNORMAL STRUCTURE AND EXPRESSION OF P53 GENE IN HUMAN HEPATOCELLULAR-CARCINOMA, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 1973 (1990).
CASSON, A. C., JOURNAL OF CELLULAR BIOCHEMISTRY 47 15F: 21 (1991).
CHANG, E, COMMUNICATION.
CHEN, R.H., EFFECT OF EXCISION REPAIR BY DIPLOID HUMAN FIBROBLASTS ON THE KINDS AND LOCATIONS OF MUTATIONS INDUCED BY (+/-)-7-BETA,8-ALPHA-DIHYDROXY-9-ALPHA,10-ALPHA-EPOXY-7,8,9,10-TETRAHYDROBENZO[A]PYRENE IN THE CODING REGION OF THE HPRT GENE, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 8680 (1990).
CHENG, J, FREQUENT MUTATIONS IN THE P53 TUMOR SUPPRESSOR GENE IN HUMAN LEUKEMIA T-CELL LINES, MOLECULAR AND CELLULAR BIOLOGY 10: 5502 (1990).
CHIBA, I, MUTATIONS IN THE P53 GENE ARE FREQUENT IN PRIMARY, RESECTED NON-SMALL-CELL LUNG-CANCER, ONCOGENE 5: 1603 (1990).
DEJONG, P.J., SPECTRUM OF SPONTANEOUS MUTATION AT THE APRT LOCUS OF CHINESE-HAMSTER OVARY CELLS - AN ANALYSIS AT THE DNA-SEQUENCE LEVEL, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 85: 3499 (1988).
Dellarco, V., Aneuploidy: Etiology and Mechanisms (1985).
DILLER, L, P53 FUNCTIONS AS A CELL-CYCLE CONTROL PROTEIN IN OSTEOSARCOMAS, MOLECULAR AND CELLULAR BIOLOGY 10: 5772 (1990).
EHRLICH, M, SPONTANEOUS DEAMINATION OF CYTOSINE AND 5-METHYLCYTOSINE RESIDUES IN DNA AND REPLACEMENT OF 5-METHYLCYTOSINE RESIDUES WITH CYTOSINE RESIDUES, MUTATION RESEARCH 238: 277 (1990).
EHRLICH, M, 5-METHYLCYTOSINE IN EUKARYOTIC DNA, SCIENCE 212: 1350 (1981).
ELIYAHU, D, METH-A FIBRO-SARCOMA CELLS EXPRESS 2 TRANSFORMING MUTANT P53 SPECIES, ONCOGENE 3: 313 (1988).
ELIYAHU, D, WILD-TYPE P53 CAN INHIBIT ONCOGENE-MEDIATED FOCUS FORMATION, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 86: 8763 (1989).
FIELDS, S, PRESENCE OF A POTENT TRANSCRIPTION ACTIVATING SEQUENCE IN THE P53 PROTEIN, SCIENCE 249: 1046 (1990).
FINLAY, C.A., THE P53 PROTO-ONCOGENE CAN ACT AS A SUPPRESSOR OF TRANSFORMATION, CELL 57: 1083 (1989).
FOSTER, P.L., BASE SUBSTITUTION MUTATIONS INDUCED BY METABOLICALLY ACTIVATED AFLATOXIN-B1, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES 80: 2695 (1983).
Gaidano, G., Proceedings of the National Academy of Sciences of the United States of America 88: 5413 (1991).
HANAWALT, P.C., PREFERENTIAL DNA-REPAIR IN EXPRESSED GENES, ENVIRONMENTAL HEALTH PERSPECTIVES 76: 9 (1987).
HARRIS, C.C., INTERINDIVIDUAL VARIATION AMONG HUMANS IN CARCINOGEN METABOLISM, DNA ADDUCT FORMATION AND DNA-REPAIR, CARCINOGENESIS 10: 1563 (1989).
HARRIS, C.C., HUMAN PULMONARY ALVEOLAR MACROPHAGES METABOLIZE BENZO(A)PYRENE TO PROXIMATE AND ULTIMATE MUTAGENS, NATURE 272: 633 (1978).
HINDS, P, MUTATION IS REQUIRED TO ACTIVATE THE P53 GENE FOR COOPERATION WITH THE RAS ONCOGENE AND TRANSFORMATION, JOURNAL OF VIROLOGY 63: 739 (1989).
HINDS, P.W., IMMUNOLOGICAL EVIDENCE FOR THE ASSOCIATION OF PARA-53 WITH A HEAT-SHOCK PROTEIN, HSC70, IN PARA-53-PLUS-RAS-TRANSFORMED CELL-LINES, MOLECULAR AND CELLULAR BIOLOGY 7: 2863 (1987).
HOLLSTEIN, M.C., FREQUENT MUTATION OF THE P53 GENE IN HUMAN ESOPHAGEAL CANCER, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 9958 (1990).
HOLLSTEIN, M.C., unpublished data.
HORSFALL, M.J., MUTATIONAL SPECIFICITY OF ALKYLATING-AGENTS AND THE INFLUENCE OF DNA-REPAIR, ENVIRONMENTAL AND MOLECULAR MUTAGENESIS 15: 107 (1990).
HOSONO, S, MOLECULAR ANALYSIS OF THE P53 ALLELES IN PRIMARY HEPATOCELLULAR CARCINOMAS AND CELL-LINES, ONCOGENE 6: 237 (1991).
HSU, I.C., MUTATIONAL HOTSPOT IN THE P53 GENE IN HUMAN HEPATOCELLULAR CARCINOMAS, NATURE 350: 427 (1991).
IGGO, R, INCREASED EXPRESSION OF MUTANT FORMS OF P53 ONCOGENE IN PRIMARY LUNG-CANCER, LANCET 335: 675 (1990).
JENKINS, J.R., 2 DISTINCT REGIONS OF THE MURINE-P53 PRIMARY AMINO-ACID SEQUENCE ARE IMPLICATED IN STABLE COMPLEX-FORMATION WITH SIMIAN VIRUS-40 T-ANTIGEN, JOURNAL OF VIROLOGY 62: 3903 (1988).
KERN, S.E., IDENTIFICATION OF P53 AS A SEQUENCE-SPECIFIC DNA-BINDING PROTEIN, SCIENCE 252: 1708 (1991).
LANE, D, COMMUNICATION.
LANE, D.P., T-ANTIGEN IS BOUND TO A HOST PROTEIN IN SV40-TRANSFORMED CELLS, NATURE 278: 261 (1979).
Lehman, T., Cancer Research 51: 4090 (1991).
LINZER, DIH, CHARACTERIZATION OF A 54K DALTON CELLULAR SV40 TUMOR-ANTIGEN PRESENT IN SV40-TRANSFORMED CELLS AND UNINFECTED EMBRYONAL CARCINOMA-CELLS, CELL 17: 43 (1979).
LOEB, L.A., MUTAGENESIS BY APURINIC APYRIMIDINIC SITES, ANNUAL REVIEW OF GENETICS 20: 201 (1986).
LOEB, L.A., ERRORS IN DNA-SYNTHESIS - A SOURCE OF SPONTANEOUS MUTATIONS, MUTATION RESEARCH 238: 297 (1990).
LUTZ, W.K., ENDOGENOUS GENOTOXIC AGENTS AND PROCESSES AS A BASIS OF SPONTANEOUS CARCINOGENESIS, MUTATION RESEARCH 238: 287 (1990).
MALKIN, D, GERM LINE P53 MUTATIONS IN A FAMILIAL SYNDROME OF BREAST-CANCER, SARCOMAS, AND OTHER NEOPLASMS, SCIENCE 250: 1233 (1990).
MARX, J.X., DETECTING MUTATIONS IN HUMAN GENES, SCIENCE 243: 737 (1989).
Mashiyama, S., Oncogene 6: 1313 (1991).
MASUDA, H, REARRANGEMENT OF THE P53 GENE IN HUMAN OSTEOGENIC SARCOMAS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 84: 7716 (1987).
MAZUR, M, SEQUENCE SPECIFICITY OF MUTATIONS INDUCED BY BENZO[ALPHA]PYRENE-7,8-DIOL-9,10-EPOXIDE AT ENDOGENOUS APRT GENE IN CHO CELLS, SOMATIC CELL AND MOLECULAR GENETICS 14: 393 (1988).
MCMAHON, G, CHARACTERIZATION OF C-KI-RAS AND N-RAS ONCOGENES IN AFLATOXIN-B1-INDUCED RAT-LIVER TUMORS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 1104 (1990).
MELLON, I, SELECTIVE REMOVAL OF TRANSCRIPTION-BLOCKING DNA DAMAGE FROM THE TRANSCRIBED STRAND OF THE MAMMALIAN DHFR GENE, CELL 51: 241 (1987).
MENON, A.G., CHROMOSOME-17P DELETIONS AND P53-GENE MUTATIONS ASSOCIATED WITH THE FORMATION OF MALIGNANT NEUROFIBROSARCOMAS IN VONRECKLINGHAUSEN NEUROFIBROMATOSIS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 5435 (1990).
MERCER, W.E., NEGATIVE GROWTH-REGULATION IN A GLIOBLASTOMA TUMOR-CELL LINE THAT CONDITIONALLY EXPRESSES HUMAN WILD-TYPE P53, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 6166 (1990).
MILLER, C.W., FREQUENCY AND STRUCTURE OF P53 REARRANGEMENTS IN HUMAN OSTEOSARCOMA, CANCER RESEARCH 50: 7950 (1990).
MILLER, J.H., MUTATIONAL SPECIFICITY IN BACTERIA, ANNUAL REVIEW OF GENETICS 17: 215 (1983).
MINNA, J, COMMUNICATION.
MUENCH, K.F., SEQUENCE SPECIFICITY IN AFLATOXIN-B1-DNA INTERACTIONS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES 80: 6 (1983).
MULLIGAN, L.M., MECHANISMS OF P53 LOSS IN HUMAN SARCOMAS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 5863 (1990).
MURAKAMI, Y, COMMUNICATION.
NIGRO, J.M., MUTATIONS IN THE P53 GENE OCCUR IN DIVERSE HUMAN-TUMOR TYPES, NATURE 342: 705 (1989).
PINHASIKIMHI, O, SPECIFIC INTERACTION BETWEEN THE P53 CELLULAR TUMOR-ANTIGEN AND MAJOR HEAT-SHOCK PROTEINS, NATURE 320: 182 (1986).
PRESTONMARTIN, S, INCREASED CELL-DIVISION AS A CAUSE OF HUMAN CANCER, CANCER RESEARCH 50: 7415 (1990).
PROSSER, J, COMMUNICATION.
PROSSER, J, EVIDENCE THAT P53 BEHAVES AS A TUMOR SUPPRESSOR GENE IN SPORADIC BREAST-TUMORS, ONCOGENE 5: 1573 (1990).
RAYCROFT, L, SCIENCE 249: 1046 (1990).
RIDEOUT, W.M., 5-METHYLCYTOSINE AS AN ENDOGENOUS MUTAGEN IN THE HUMAN LDL RECEPTOR AND P53 GENES, SCIENCE 249: 1288 (1990).
RODRIGUES, N.R., P53 MUTATIONS IN COLORECTAL-CANCER, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 7555 (1990).
ROMANO, J.W., IDENTIFICATION AND CHARACTERIZATION OF A P53 GENE MUTATION IN A HUMAN OSTEO-SARCOMA CELL-LINE, ONCOGENE 4: 1483 (1989).
SARNOW, P, ADENOVIRUS E1B-58KD TUMOR-ANTIGEN AND SV40 LARGE TUMOR-ANTIGEN ARE PHYSICALLY ASSOCIATED WITH THE SAME 54 KD CELLULAR PROTEIN IN TRANSFORMED-CELLS, CELL 28: 387 (1982).
SHIBUTANI, S, INSERTION OF SPECIFIC BASES DURING DNA-SYNTHESIS PAST THE OXIDATION-DAMAGED BASE 8-OXODG, NATURE 349: 431 (1991).
SHIGENAGA, M.K., URINARY 8-HYDROXY-2'-DEOXYGUANOSINE AS A BIOLOGICAL MARKER OF INVIVO OXIDATIVE DNA DAMAGE, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 86: 9697 (1989).
SOUSSI, T, STRUCTURAL ASPECTS OF THE P53 PROTEIN IN RELATION TO GENE EVOLUTION, ONCOGENE 5: 945 (1990).
SRIVASTAVA, S, GERM-LINE TRANSMISSION OF A MUTATED P53 GENE IN A CANCER-PRONE FAMILY WITH LI-FRAUMENI SYNDROME, NATURE 348: 747 (1990).
STURZBECHER, H.W., MUTANT P53 PROTEINS BIND HSP 72/73 CELLULAR HEAT SHOCK-RELATED PROTEINS IN SV40-TRANSFORMED MONKEY CELLS, ONCOGENE 1: 201 (1987).
TAKAHASHI, T, P53 - A FREQUENT TARGET FOR GENETIC ABNORMALITIES IN LUNG-CANCER, SCIENCE 246: 491 (1989).
THEILLET, C, COMMUNICATION.
THILLY, W.G., MUTATIONAL SPECTROMETRY IN ANIMAL TOXICITY TESTING, ANNUAL REVIEW OF PHARMACOLOGY AND TOXICOLOGY 30: 369 (1990).
VOGELSTEIN, B, CANCER - A DEADLY INHERITANCE, NATURE 348: 681 (1990).
VOGELSTEIN, B, unpublished data.
WERNESS, B.A., ASSOCIATION OF HUMAN PAPILLOMAVIRUS TYPE-16 AND TYPE-18 E6 PROTEINS WITH P53, SCIENCE 248: 76 (1990).
WIEBAUER, K, MISMATCH-SPECIFIC THYMINE DNA GLYCOSYLASE AND DNA POLYMERASE-BETA MEDIATE THE CORRECTION OF G.T MISPAIRS IN NUCLEAR EXTRACTS FROM HUMAN-CELLS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 87: 5842 (1990).
WILD, C.P., AFLATOXIN ALBUMIN ADDUCTS IN HUMAN SERA FROM DIFFERENT REGIONS OF THE WORLD, CARCINOGENESIS 11: 2271 (1990).
WILLETT, W, THE SEARCH FOR THE CAUSES OF BREAST AND COLON CANCER, NATURE 338: 389 (1989).
WOGAN, G.N., MARKERS OF EXPOSURE TO CARCINOGENS, ENVIRONMENTAL HEALTH PERSPECTIVES 81: 9 (1989).
WOLF, D, MAJOR DELETIONS IN THE GENE ENCODING THE P53 TUMOR-ANTIGEN CAUSE LACK OF P53 EXPRESSION IN HL-60 CELLS, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 82: 790 (1985).
WOOD, M.L., MECHANISTIC STUDIES OF IONIZING-RADIATION AND OXIDATIVE MUTAGENESIS - GENETIC-EFFECTS OF A SINGLE 8-HYDROXYGUANINE (7-HYDRO-8-OXOGUANINE) RESIDUE INSERTED AT A UNIQUE SITE IN A VIRAL GENOME, BIOCHEMISTRY 29: 7024 (1990).
YOU, M, ACTIVATION OF THE KI-RAS PROTOONCOGENE IN SPONTANEOUSLY OCCURRING AND CHEMICALLY-INDUCED LUNG-TUMORS OF THE STRAIN-A MOUSE, PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA 86: 3070 (1989).
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Volume 253 | Issue 5015
5 July 1991
5 July 1991
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