Expression of wild-type p53 is not compatible with continued growth of p53-negative tumor cells. | Zendy

Peter Johnson | Zendy; David Gray | Zendy; Michael Mowat | Zendy; Samuel Benchimol | Zendy

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Expression of wild-type p53 is not compatible with continued growth of p53-negative tumor cells.

Author(s) -

Peter Johnson,

David Gray,

Michael Mowat,

Samuel Benchimol

Publication year - 1991

Publication title -

molecular and cellular biology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.14

H-Index - 327

eISSN - 1067-8824

pISSN - 0270-7306

DOI - 10.1128/mcb.11.1.1

Subject(s) - biology , transfection , carcinogenesis , tumor suppressor gene , wild type , k562 cells , gene , cell culture , cancer research , mutation , suppressor , microbiology and biotechnology , genetics , mutant

Inactivation of the cellular p53 gene is a common feature of Friend virus-induced murine erythroleukemia cell lines and may represent a necessary step in the progression of this disease. As well, frequent loss or mutation of p53 alleles in diverse human tumors is consistent with the view of p53 as a tumor suppressor gene. To examine the significance of p53 gene inactivation in tumorigenesis, we have attempted to express transfected wild-type p53 in three p53-negative tumor cell lines: murine DP16-1 Friend erythroleukemia cells, human K562 cells, and SKOV-3 cells. We found that aberrant p53 proteins, which differ from wild-type p53 by a single amino acid substitution, were expressed stably in these cells, whereas wild-type p53 expression was not tolerated. The inability of p53-negative tumor cell lines to support long-term expression of wild-type p53 protein is consistent with the view that p53 is a tumor suppressor gene.

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