TY - JOUR
T1 - The p63 C-terminus is essential for murine oocyte integrity
AU - Lena, Anna Maria
AU - Rossi, Valerio
AU - Osterburg, Susanne
AU - Smirnov, Artem
AU - Osterburg, Christian
AU - Tuppi, Marcel
AU - Cappello, Angela
AU - Amelio, Ivano
AU - Dötsch, Volker
AU - De Felici, Massimo
AU - Klinger, Francesca Gioia
AU - Annicchiarico-Petruzzelli, Margherita
AU - Valensise, Herbert
AU - Melino, Gerry
AU - Candi, Eleonora
N1 - Funding Information:
This work has been mainly supported by AIRC Grants (IG-22206 to E.C.) and Ministry of Health and Fondazione Luigi Maria Monti IDI-RCCS (RC to E.C.). The work was also partially supported by AIRC (IG#20473, 2017-2022; Start-up ID23219, 2019-2024). V.D. acknowledges support by DFG (DO 545/20-1).
Publisher Copyright:
© 2021, The Author(s).
PY - 2021/12
Y1 - 2021/12
N2 - The transcription factor p63 mediates distinct cellular responses, primarily regulating epithelial and oocyte biology. In addition to the two amino terminal isoforms, TAp63 and ΔNp63, the 3’-end of p63 mRNA undergoes tissue-specific alternative splicing that leads to several isoforms, including p63α, p63β and p63γ. To investigate in vivo how the different isoforms fulfil distinct functions at the cellular and developmental levels, we developed a mouse model replacing the p63α with p63β by deletion of exon 13 in the Trp63 gene. Here, we report that whereas in two organs physiologically expressing p63α, such as thymus and skin, no abnormalities are detected, total infertility is evident in heterozygous female mice. A sharp reduction in the number of primary oocytes during the first week after birth occurs as a consequence of the enhanced expression of the pro-apoptotic transcriptional targets Puma and Noxa by the tetrameric, constitutively active, TAp63β isoform. Hence, these mice show a condition of ovary dysfunction, resembling human primary ovary insufficiency. Our results show that the p63 C-terminus is essential in TAp63α-expressing primary oocytes to control cell death in vivo, expanding the current understanding of human primary ovarian insufficiency.
AB - The transcription factor p63 mediates distinct cellular responses, primarily regulating epithelial and oocyte biology. In addition to the two amino terminal isoforms, TAp63 and ΔNp63, the 3’-end of p63 mRNA undergoes tissue-specific alternative splicing that leads to several isoforms, including p63α, p63β and p63γ. To investigate in vivo how the different isoforms fulfil distinct functions at the cellular and developmental levels, we developed a mouse model replacing the p63α with p63β by deletion of exon 13 in the Trp63 gene. Here, we report that whereas in two organs physiologically expressing p63α, such as thymus and skin, no abnormalities are detected, total infertility is evident in heterozygous female mice. A sharp reduction in the number of primary oocytes during the first week after birth occurs as a consequence of the enhanced expression of the pro-apoptotic transcriptional targets Puma and Noxa by the tetrameric, constitutively active, TAp63β isoform. Hence, these mice show a condition of ovary dysfunction, resembling human primary ovary insufficiency. Our results show that the p63 C-terminus is essential in TAp63α-expressing primary oocytes to control cell death in vivo, expanding the current understanding of human primary ovarian insufficiency.
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U2 - 10.1038/s41467-020-20669-0
DO - 10.1038/s41467-020-20669-0
M3 - Article
C2 - 33452256
AN - SCOPUS:85099465130
SN - 2041-1723
VL - 12
JO - Nature Communications
JF - Nature Communications
IS - 1
M1 - 383
ER -