Endogenous p53 gene status predicts the response of human squamous cell carcinomas to wild-type p53

被引:0
|
作者
Lisa S St. John
Edward R Sauter
Meenhard Herlyn
Samuel Litwin
Karen Adler-Storthz
机构
[1] Dental Branch,Department of Basic Sciences
[2] Graduate School of Biomedical Sciences,Department of Biostatistics
[3] University of Texas-Houston Health Science Center,undefined
[4] The Wistar Institute,undefined
[5] Fox Chase Cancer Center,undefined
来源
Cancer Gene Therapy | 2000年 / 7卷
关键词
p53; squamous cell carcinoma; growth arrest; apoptosis; WAF1; WAF1; p21.;
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中图分类号
学科分类号
摘要
Prior reports suggest that p53 protein status may influence the response to gene transduction with wild-type (wt) p53. Adenoviral vectors containing the p53 gene were administered to normal keratinocytes, to squamous cell carcinoma (SCC) lines with varied p53 protein status (absent, mutant, wt, or degraded by papillomavirus), as well as to tumors formed in severe combined immunodeficient mice. The percentage of cells undergoing apoptosis, G1 growth arrest, WAF1/p21 induction, and in vivo tumor progression were studied after wt p53 gene transduction. Apoptosis developed first in normal keratinocytes, next in SCCs lacking p53 protein, and last in SCCs with mutant or degraded p53 protein. All of the cell lines studied demonstrated an increase in WAF1/p21 protein, but only those lacking p53 protein showed G1 arrest. Tumors lacking p53 protein were more susceptible to p53 overexpression than those containing mutant or degraded p53 protein. The endogenous p53 protein status of SCCs appears to influence the outcome of p53 gene transduction.
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页码:749 / 756
页数:7
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