4.8 Article

p53 mutant mice that display early ageing-associated phenotypes

Journal

NATURE
Volume 415, Issue 6867, Pages 45-53

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NATURE PUBLISHING GROUP
DOI: 10.1038/415045a

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The p53 tumour suppressor is activated by numerous stressors to induce apoptosis, cell cycle arrest, or senescence. To study the biological effects of altered p53 function, we generated mice with a deletion mutation in the first six exons of the p53 gene that express a truncated RNA capable of encoding a carboxy-terminal p53 fragment. This mutation confers phenotypes consistent with activated p53 rather than inactivated p53. Mutant (p53(+/m)) mice exhibit enhanced resistance to spontaneous tumours compared with wild-type (p53(+/+)) littermates. As p53(+/)m mice age, they display an early onset of phenotypes associated with ageing. These include reduced longevity, osteoporosis, generalized organ atrophy and a diminished stress tolerance. A second line of transgenic mice containing a temperature-sensitive mutant allele of p53 also exhibits early ageing phenotypes. These data suggest that p53 has a role in regulating organismal ageing.

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