Deletion of p63 exon 13 in mice reveals C-terminal functions in
成果类型:
Article
署名作者:
Lena, Anna Maria; Smirnov, Artem; Mancini, Mara; Montanaro, Manuela; Ciccosanti, Fabiola; Foti, Valeria; Nardacci, Roberta; Fimia, Gian Maria; Mavilio, Mara; Federici, Massimo; Mauriello, Alessandro; Piacentini, Mauro; Melino, Gerry; Candi, Eleonora
署名单位:
University of Rome Tor Vergata; University of Rome Tor Vergata
刊物名称:
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
ISSN/ISSBN:
0027-8939
DOI:
10.1073/pnas.2503866122
发表日期:
2025-07-22
关键词:
epithelial development
p53 homolog
dna-damage
enhancers
delta-np63-alpha
regulator
apoptosis
isoforms
residues
protects
摘要:
The transcription factor p63 is an essential regulator of epithelial development. Yet, the complexity at the 3 ' UTR, which gives rise to the three distinct C-terminal protein isoforms (alpha, f3, and gamma), remains unresolved and opens an investigation on the in vivo role of the C-terminus. This region, codified by exon 13, harbors genetic mutations leading to AEC syndrome. Here, we generated a mouse with a deletion of p63 exon 13 in keratin-14-expressing tissues and employed transcriptome, genome-wide occupancy, and interactome studies to characterize the role of the p63 C-terminus in vivo. In this model mouse, the p63 protein is expressed at the correct level in time and space but predominantly as the f3 isoform instead of the alpha isoform, thereby providing insights into the function of the C-terminus. We show that p63f3 interacts more readily with the core promoter transcription machinery and p63 alpha- depleted isoforms bind more frequently the promoter region of target genes, resulting in inappropriate overexpression of extracellular matrix organization genes in the skin. This leads to the aberrant adhesion of epidermal keratinocytes to the basal lamina and triggers systemic inflammation, growth abnormalities, and premature death. We found a significant role of the full-length ONp63a isoform which cannot be substituted by the other isoforms (f3 or gamma). Our studies highlight a crucial role for p63 alpha in correctly orchestrating the gene expression program to ensure proper formation of epithelia.
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