Dominant-negative but not gain-of-function effects of a p53.R270H mutation in mouse epithelium tissue after DNA damage.

نویسندگان

  • Susan W P Wijnhoven
  • Ewoud N Speksnijder
  • Xiaoling Liu
  • Edwin Zwart
  • Conny Th M vanOostrom
  • Rudolf B Beems
  • Esther M Hoogervorst
  • Mirjam M Schaap
  • Laura D Attardi
  • Tyler Jacks
  • Harry van Steeg
  • Jos Jonkers
  • Annemieke de Vries
چکیده

p53 alterations in human tumors often involve missense mutations that may confer dominant-negative or gain-of-function properties. Dominant-negative effects result in inactivation of wild-type p53 protein in heterozygous mutant cells and as such in a p53 null phenotype. Gain-of-function effects can directly promote tumor development or metastasis through antiapoptotic mechanisms or transcriptional activation of (onco)genes. Here, we show, using conditional mouse technology, that epithelium-specific heterozygous expression of mutant p53 (i.e., the p53.R270H mutation that is equivalent to the human hotspot R273H) results in an increased incidence of spontaneous and UVB-induced skin tumors. Expression of p53.R270H exerted dominant-negative effects on latency, multiplicity, and progression status of UVB-induced but not spontaneous tumors. Surprisingly, gain-of-function properties of p53.R270H were not detected in skin epithelium. Apparently, dominant-negative and gain-of-function effects of mutant p53 are highly tissue specific and become most manifest upon stabilization of p53 after DNA damage.

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عنوان ژورنال:
  • Cancer research

دوره 67 10  شماره 

صفحات  -

تاریخ انتشار 2007