| Literature DB >> 31322742 |
Yuezhen Xue1, Boris San Luis1, David P Lane1.
Abstract
Genomic alterations in different types of cancer have been identified by comprehensive sequencing methodologies, revealing TP53 as the most frequently mutated gene across the majority of human cancer types. Cytotoxic treatments are still major cancer therapy strategies but cancer recurrence due to therapy resistance is a major challenge. Resistant cell populations may be associated with TP53 mutant clones exhibiting abnormal p53 expression patterns in tumours. Given data that levels of mutant p53 influence cancer cell growth and survival, understanding the mechanisms underlying intratumour heterogeneity of p53 can be exploited to design strategies that improve patient survival. The patterns of p53 protein examined by immunohistochemistry of both premalignant and malignant tissues are complex, ranging from intense staining of all tumour cell nuclei to complete absence of staining and with many intermediate phenotypes. Animal models that express only mutant proteins and adoption of international standards for terminology have brought greater clarity to understanding the causes of variation and are at the same time demonstrating the utility of p53 in oncology. In addition to p53 mutation, MDM2 and chaperone activities, gene copy number and TP53 mRNA levels linked to proliferative activity and differentiation are all now established as causes of variation in p53 staining, with clinical implications.Entities:
Keywords: HSP70; HSP90; MDM2; cell differentiation; colorectal cancer; epigenetics; immunohistochemistry; intratumour heterogeneity; p53; retinoblastoma; skin squamous cell carcinomas; transcriptional regulation
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Year: 2019 PMID: 31322742 DOI: 10.1002/path.5328
Source DB: PubMed Journal: J Pathol ISSN: 0022-3417 Impact factor: 7.996