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Mutations in the p53 gene occur in diverse human tumour types View Full Text

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Article Info

DATE

1989-12

AUTHORS

Janice M. Nigro, Suzanne J. Baker, Antonette C. Preisinger, J. Milburn Jessup, Richard Hosteller, Karen Cleary, Sandra H. Signer, Nancy Davidson, Stephen Baylin, Peter Devilee, Thomas Glover, Francis S. Collins, Ainsley Weslon, Rama Modali, Curtis C. Harris, Bert Vogelstein

ABSTRACT

THE p53 gene has been a constant source of fascination since its discovery nearly a decade ago1,2. Originally considered to be an oncogene, several convergent lines of research have indicated that the wild-type gene product actually functions as a tumour suppressor gene3–9. For example, expression of the neoplastic phenotype is inhibited, rather than promoted, when rat cells are transfected with the murine wild-type p53 gene together with mutant p53 genes and/or other oncogenes3,4. Moreover, in human tumours, the short arm of chromosome 17 is often deleted (reviewed in ref. 10). In colorectal cancers, the smallest common region of deletion is centred at 17pl3.1 (ref. 9); this region harbours the p53 gene, and in two tumours examined in detail, the remaining (non-deleted) p53 alleles were found to contain mutations9. This result was provocative because allelic deletion coupled with mutation of the remaining allele is a theoretical hallmark of tumour-suppressor genes11. In the present report, we have attempted to determine the generality of this observation; that is, whether tumours with allelic deletions of chromosome 17p contain mutant p53 genes in the allele that is retained. Our results suggest that (1) most tumours with such allelic deletions contain p53 point mutations resulting in amino-acid substitutions, (2) such mutations are not confined to tumours with allelic deletion, but also occur in at least some tumours that have retained both parental 17p alleles, and (3) p53 gene mutations are clustered in four 'hot-spots' which exactly coincide with the four most highly conserved regions of the gene. These results suggest that p53 mutations play a role in the development of many common human malignancies. More... »

PAGES

705-708

References to SciGraph publications

  • 1987-09. Functional inactivation of genes by dominant negative mutations in NATURE
  • 1979-03. T antigen is bound to a host protein in SY40-transformed cells in NATURE

    • Journal

    TITLE

    Nature

    ISSUE

    6250

    VOLUME

    342

    Subjects

  • FOR: Biological Sciences
  • FOR: Genetics
  • MESH: Alleles
  • MESH: Base Sequence
  • MESH: Chromosome Deletion
  • MESH: Chromosomes, Human, Pair 17
  • MESH: Cloning, Molecular
  • MESH: Codon
  • MESH: Dna, Neoplasm
  • MESH: Dna-Directed Dna Polymerase
  • MESH: Humans
  • MESH: Molecular Sequence Data
  • MESH: Mutation
  • MESH: Neoplasms
  • MESH: Neurofibromatosis 1
  • MESH: Oncogene Proteins
  • MESH: Phosphoproteins
  • MESH: Rna, Messenger
  • MESH: Tumor Suppressor Protein P53

    • Author Affiliations

  • The Johns Hopkins Oncology Center, 424 North Bond Street, 21231, Baltimore, Maryland, USA
  • M. D. Anderson Hospital, 77030, Houston, Texas, USA
  • Department of Pathology, Duke University, 27710, Durham, North Carolina, USA
  • Department of Human Genetics, University of Leiden, Holland
  • Department of Human Genetics, University of Michigan, 48109, Ann Arbor, Michigan, USA
  • Laboratory of Human Carcinogenesis, National Cancer Institute, 20892, Bethesda, Maryland, USA

    • Related Patents

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    • Identifiers

    URI

    http://scigraph.springernature.com/pub.10.1038/342705a0

    DOI

    http://dx.doi.org/10.1038/342705a0

    DIMENSIONS

    https://app.dimensions.ai/details/publication/pub.1041126170

    PUBMED

    https://www.ncbi.nlm.nih.gov/pubmed/2531845

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