Germ-line Mutations of the P53 Tumor Suppressor Gene in Patients with High Risk for Cancer Inactivate the P53 Protein

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 1992 Jul 15

PMID 1631137

Citations 26

Authors

T Frebourg

J Kassel

K T Lam

M A Gryka

N Barbier

T I Andersen

A L Borresen

S H Friend

Affiliations

Soon will be listed here.

Abstract

Germ-line mutations in the p53 tumor suppressor gene have been observed in patients with Li-Fraumeni syndrome, brain tumors, second malignancies, and breast cancers. It is unclear whether all of these mutations have inactivated p53 and thereby provide an increased risk for cancer. Therefore, it is necessary to establish the biological significance of these germ-line mutations by the functional and structural analysis of the resulting mutant p53 proteins. We analyzed the ability of seven germ-line mutant proteins observed in patients with Li-Fraumeni syndrome, second primary neoplasms, or familial breast cancer to block the growth of malignant cells and compared the structural properties of the mutant proteins to that of the wild-type protein. Six of seven missense mutations disrupted the growth inhibitory properties and structure of the wild-type protein. One germ-line mutation retained the features of the wild-type p53. Genetic analysis of the breast cancer family in which this mutation was observed indicated that this germ-line mutation was not associated with the development of cancer. These results demonstrate that germ-line p53 mutations observed in patients with Li-Fraumeni syndrome and with second malignancies have inactivated the p53 tumor suppressor gene. The inability of the germ-line p53 mutants to block the growth of malignant cells can explain why patients with these germ-line mutations have an increased risk for cancer. The observation of a functionally silent germ-line mutation indicates that, before associating a germ-line tumor suppressor gene mutation with cancer risk, it is prudent to consider its functional significance.

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References

Hinds P, Finlay C, Quartin R, Baker S, Fearon E, Vogelstein B . Mutant p53 DNA clones from human colon carcinomas cooperate with ras in transforming primary rat cells: a comparison of the "hot spot" mutant phenotypes. Cell Growth Differ. 1990; 1(12):571-80. View

Li F, Fraumeni Jr J . Rhabdomyosarcoma in children: epidemiologic study and identification of a familial cancer syndrome. J Natl Cancer Inst. 1969; 43(6):1365-73. View

Caron de Fromentel C, Soussi T . TP53 tumor suppressor gene: a model for investigating human mutagenesis. Genes Chromosomes Cancer. 1992; 4(1):1-15. DOI: 10.1002/gcc.2870040102. View

Borresen A, Andersen T, Garber J, Thorlacius S, Eyfjord J, Ottestad L . Screening for germ line TP53 mutations in breast cancer patients. Cancer Res. 1992; 52(11):3234-6. View

Sidransky D, Tokino T, Helzlsouer K, Zehnbauer B, Rausch G, Shelton B . Inherited p53 gene mutations in breast cancer. Cancer Res. 1992; 52(10):2984-6. View

Malkin D, Jolly K, Barbier N, Look A, Friend S, Gebhardt M . Germline mutations of the p53 tumor-suppressor gene in children and young adults with second malignant neoplasms. N Engl J Med. 1992; 326(20):1309-15. DOI: 10.1056/NEJM199205143262002. View

Toguchida J, Yamaguchi T, Dayton S, Beauchamp R, Herrera G, Ishizaki K . Prevalence and spectrum of germline mutations of the p53 gene among patients with sarcoma. N Engl J Med. 1992; 326(20):1301-8. DOI: 10.1056/NEJM199205143262001. View

Metzger A, Sheffield V, Duyk G, Daneshvar L, Edwards M, Cogen P . Identification of a germ-line mutation in the p53 gene in a patient with an intracranial ependymoma. Proc Natl Acad Sci U S A. 1991; 88(17):7825-9. PMC: 52396. DOI: 10.1073/pnas.88.17.7825. View

Law J, Strong L, Chidambaram A, Ferrell R . A germ line mutation in exon 5 of the p53 gene in an extended cancer family. Cancer Res. 1991; 51(23 Pt 1):6385-7. View

10.

Casey G, Lopez M, Vogelstein B, Stanbridge E . Growth suppression of human breast cancer cells by the introduction of a wild-type p53 gene. Oncogene. 1991; 6(10):1791-7. View

11.

Hollstein M, Sidransky D, Vogelstein B, Harris C . p53 mutations in human cancers. Science. 1991; 253(5015):49-53. DOI: 10.1126/science.1905840. View

12.

Isaacs W, Carter B, Ewing C . Wild-type p53 suppresses growth of human prostate cancer cells containing mutant p53 alleles. Cancer Res. 1991; 51(17):4716-20. View

13.

Kern S, Kinzler K, Bruskin A, Jarosz D, Friedman P, Prives C . Identification of p53 as a sequence-specific DNA-binding protein. Science. 1991; 252(5013):1708-11. DOI: 10.1126/science.2047879. View

14.

Levine A, Momand J, Finlay C . The p53 tumour suppressor gene. Nature. 1991; 351(6326):453-6. DOI: 10.1038/351453a0. View

15.

Georgoff I, Martinez J, Levine A . Cellular localization and cell cycle regulation by a temperature-sensitive p53 protein. Genes Dev. 1991; 5(2):151-9. DOI: 10.1101/gad.5.2.151. View

16.

Johnson P, Gray D, Mowat M, Benchimol S . Expression of wild-type p53 is not compatible with continued growth of p53-negative tumor cells. Mol Cell Biol. 1991; 11(1):1-11. PMC: 359576. DOI: 10.1128/mcb.11.1.1-11.1991. View

17.

Malkin D, Li F, Strong L, Fraumeni Jr J, Nelson C, Kim D . Germ line p53 mutations in a familial syndrome of breast cancer, sarcomas, and other neoplasms. Science. 1990; 250(4985):1233-8. DOI: 10.1126/science.1978757. View

18.

Srivastava S, Zou Z, Pirollo K, Blattner W, Chang E . Germ-line transmission of a mutated p53 gene in a cancer-prone family with Li-Fraumeni syndrome. Nature. 1990; 348(6303):747-9. DOI: 10.1038/348747a0. View

19.

Diller L, Kassel J, Nelson C, Gryka M, Litwak G, Gebhardt M . p53 functions as a cell cycle control protein in osteosarcomas. Mol Cell Biol. 1990; 10(11):5772-81. PMC: 361354. DOI: 10.1128/mcb.10.11.5772-5781.1990. View

20.

Brown M, Figge J, Hansen U, Wright C, Jeang K, Khoury G . lac repressor can regulate expression from a hybrid SV40 early promoter containing a lac operator in animal cells. Cell. 1987; 49(5):603-12. DOI: 10.1016/0092-8674(87)90536-8. View