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The C terminus of p73 is essential for hippocampal development

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2020

Autor:innen

Panatta, Emanuele
Niklison-Chirou, Maria Victoria
Steinert, Joern R.
Agostini, Massimiliano
Morone, Nobuhiro
Knight, Richard A.
Melino, Gerry

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Proceedings of the National Academy of Sciences of the United States of America. National Academy of Sciences. 2020, 117(27), pp. 15694-15701. ISSN 0027-8424. eISSN 1091-6490. Available under: doi: 10.1073/pnas.2000917117

Zusammenfassung

The p53 family member p73 has a complex gene structure, including alternative promoters and alternative splicing of the 3' UTR. This results in a complex range of isoforms whose biological relevance largely remains to be determined. By deleting exon 13 (which encodes a sterile α motif) from the Trp73 gene, we selectively engineered mice to replace the most abundantly expressed C-terminal isoform, p73α, with a shorter product of alternative splicing, p73β. These mice (Trp73 Δ13/Δ13 ) display severe neurodevelopmental defects with significant functional and morphological abnormalities. Replacement of p73α with p73β results in the depletion of Cajal-Retzius (CR) cells in embryonic stages, thus depriving the developing hippocampus of the pool of neurons necessary for correct hippocampal architecture. Consequently, Trp73 Δ13/Δ13 mice display severe hippocampal dysgenesis, reduced synaptic functionality and impaired learning and memory capabilities. Our data shed light on the relevance of p73 alternative splicing and show that the full-length C terminus of p73 is essential for hippocampal development.

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570 Biowissenschaften, Biologie

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p53 family, neurodevelopment, alternative splicing

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ISO 690AMELIO, Ivano, Emanuele PANATTA, Maria Victoria NIKLISON-CHIROU, Joern R. STEINERT, Massimiliano AGOSTINI, Nobuhiro MORONE, Richard A. KNIGHT, Gerry MELINO, 2020. The C terminus of p73 is essential for hippocampal development. In: Proceedings of the National Academy of Sciences of the United States of America. National Academy of Sciences. 2020, 117(27), pp. 15694-15701. ISSN 0027-8424. eISSN 1091-6490. Available under: doi: 10.1073/pnas.2000917117
BibTex
@article{Amelio2020termi-57061,
  year={2020},
  doi={10.1073/pnas.2000917117},
  title={The C terminus of p73 is essential for hippocampal development},
  number={27},
  volume={117},
  issn={0027-8424},
  journal={Proceedings of the National Academy of Sciences of the United States of America},
  pages={15694--15701},
  author={Amelio, Ivano and Panatta, Emanuele and Niklison-Chirou, Maria Victoria and Steinert, Joern R. and Agostini, Massimiliano and Morone, Nobuhiro and Knight, Richard A. and Melino, Gerry}
}
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    <dcterms:abstract xml:lang="eng">The p53 family member p73 has a complex gene structure, including alternative promoters and alternative splicing of the 3' UTR. This results in a complex range of isoforms whose biological relevance largely remains to be determined. By deleting exon 13 (which encodes a sterile α motif) from the Trp73 gene, we selectively engineered mice to replace the most abundantly expressed C-terminal isoform, p73α, with a shorter product of alternative splicing, p73β. These mice (Trp73 &lt;sup&gt;Δ13/Δ13&lt;/sup&gt; ) display severe neurodevelopmental defects with significant functional and morphological abnormalities. Replacement of p73α with p73β results in the depletion of Cajal-Retzius (CR) cells in embryonic stages, thus depriving the developing hippocampus of the pool of neurons necessary for correct hippocampal architecture. Consequently, Trp73&lt;sup&gt; Δ13/Δ13&lt;/sup&gt; mice display severe hippocampal dysgenesis, reduced synaptic functionality and impaired learning and memory capabilities. Our data shed light on the relevance of p73 alternative splicing and show that the full-length C terminus of p73 is essential for hippocampal development.</dcterms:abstract>
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