posted on 2023-05-17, 13:01authored byCraig, AL, Holcakova, J, Finlan, LE, Nekulova, M, Hrstka, R, Nuri GuvenNuri Guven, Smith, G, DiRenzo, J, Hupp, TR, Vojtesek, B
Abstract Background: ÄNp63á is an epithelial progenitor cell marker that maintains epidermal stem cell self-renewal capacity.Previous studies revealed that UV-damage induced p53 phosphorylation is confined to ÄNp63á-positive cells in the basal layer of human epithelium. Results: We now report that phosphorylation of the p53 tumour suppressor is positively regulated by ÄNp63á in immortalised human keratinocytes. ÄNp63á depletion by RNAi reduces steady-state ATM mRNA and protein levels, and attenuates p53 Serine-15 phosphorylation. Conversely, ectopic expression of ÄNp63á in p63-null tumour cells stimulates ATM transcription and p53 Serine-15 phosphorylation. We show that ATM is a direct ÄNp63á transcriptional target and that the ÄNp63á response element localizes to the ATM promoter CCAAT sequence. Structure-function analysis revealed that the ÄNp63-specific TA2 transactivation domain mediates ATM transcription in coordination with the DNA binding and SAM domains. Conclusions: Germline p63 point mutations are associated with a range of ectodermal developmental disorders, and targeted p63 deletion in the skin causes premature ageing. The ÄNp63á-ATM-p53 damage-response pathway may therefore function in epithelial development, carcinogenesis and the ageing processes.
History
Publication title
Molecular Cancer
Volume
9
Issue
195
Pagination
1-13
ISSN
1476-4598
Department/School
School of Pharmacy and Pharmacology
Publisher
BioMed Central Ltd.
Place of publication
UK
Rights statement
Licenced under Creative Commons Attribution 2.0 Generic (CC BY 2.0) http://creativecommons.org/licenses/by/2.0/