Aging normal human oesophagus accumulates TP53 mutant clones. These are the origin of most oesophageal squamous carcinomas, in which biallelic TP53 disruption is almost universal. However, how p53 mutant clones expand and contribute to cancer development is unclear. Here we show that inducing the p53R245W mutant in single oesophageal progenitor cells in transgenic mice confers a proliferative advantage and clonal expansion but does not disrupt normal epithelial structure. Loss of the remaining p53 allele in mutant cells results in genomically unstable p53R245W/null epithelium with giant polyaneuploid cells and copy number altered clones. In carcinogenesis, p53 mutation does not initiate tumour formation, but tumours developing from areas wi...
Wild-type p53 functions as a tumour suppressor while mutant p53 possesses oncogenic potential. Until...
Mutations in the p53 tumor suppressor gene are found in over 50% of human tumors and in the germline...
The extent to which cells in normal tissues accumulate mutations throughout life is poorly understoo...
Funder: MRC Cancer unitFunder: Clare CollegeDuring ageing, normal epithelial tissues progressively a...
During ageing, normal epithelial tissues progressively accumulate clones carrying mutations that inc...
During aging, progenitor cells acquire mutations, which may generate clones that colonize the surrou...
Summary: p53 is a tumor suppressor protein, and its missense mutations are frequently found in human...
We examined the selective pressure for, and the impact of, p53 inactivation during epithelial tumor ...
The timing of p53 mutation in the multistep process of esophageal carcinogenesis is still under deba...
The extent to which cells in normal tissues accumulate mutations throughout life is poorly understoo...
p53 (TP53) is the most commonly mutated tumor suppressor in cancer. How mutant forms of p53 can cont...
Pancreatic cancer is characterized by nearly universal activating mutations in KRAS. Among other som...
We examined the selective pressure for, and the impact of, p53 inactivation during epithelial tumor ...
BACKGROUND: The p53 tumor suppressor gene is mutated in a large percentage of human malignancies, in...
Nasopharyngeal carcinoma (NPC) is a malignancy which is consistently associated with the Epstein-Bar...
Wild-type p53 functions as a tumour suppressor while mutant p53 possesses oncogenic potential. Until...
Mutations in the p53 tumor suppressor gene are found in over 50% of human tumors and in the germline...
The extent to which cells in normal tissues accumulate mutations throughout life is poorly understoo...
Funder: MRC Cancer unitFunder: Clare CollegeDuring ageing, normal epithelial tissues progressively a...
During ageing, normal epithelial tissues progressively accumulate clones carrying mutations that inc...
During aging, progenitor cells acquire mutations, which may generate clones that colonize the surrou...
Summary: p53 is a tumor suppressor protein, and its missense mutations are frequently found in human...
We examined the selective pressure for, and the impact of, p53 inactivation during epithelial tumor ...
The timing of p53 mutation in the multistep process of esophageal carcinogenesis is still under deba...
The extent to which cells in normal tissues accumulate mutations throughout life is poorly understoo...
p53 (TP53) is the most commonly mutated tumor suppressor in cancer. How mutant forms of p53 can cont...
Pancreatic cancer is characterized by nearly universal activating mutations in KRAS. Among other som...
We examined the selective pressure for, and the impact of, p53 inactivation during epithelial tumor ...
BACKGROUND: The p53 tumor suppressor gene is mutated in a large percentage of human malignancies, in...
Nasopharyngeal carcinoma (NPC) is a malignancy which is consistently associated with the Epstein-Bar...
Wild-type p53 functions as a tumour suppressor while mutant p53 possesses oncogenic potential. Until...
Mutations in the p53 tumor suppressor gene are found in over 50% of human tumors and in the germline...
The extent to which cells in normal tissues accumulate mutations throughout life is poorly understoo...