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Publication : Distinct function of P63 isoforms during embryonic skeletal development.

First Author  Lu Y Year  2013
Journal  Gene Volume  519
Issue  2 Pages  251-9
PubMed ID  23481305 Mgi Jnum  J:196359
Mgi Id  MGI:5487838 Doi  10.1016/j.gene.2013.02.021
Citation  Lu Y, et al. (2013) Distinct function of P63 isoforms during embryonic skeletal development. Gene 519(2):251-9
abstractText  P63 belongs to the P53 family of transcription factors. There are multiple P63 isoforms that play important functions both in cancer and development. The obvious limb defect in p63 null mice and in human skeletal syndromes with P63 mutations suggest its essential role in long bone development. However, how the different P63 isoforms function during long bone development is largely unknown. We have previously shown that TAP63alpha, the longest P63 isoform, plays a positive role in embryonic skeletal development, since targeting TAP63alpha expression in hypertrophic chondrocytes accelerates endochondral ossification at both E17.5 and P1 stages. Here, we report transgenic studies of DeltaNP63alpha, another P63 isoform which lacks the N-terminal transactivation domain compared to TAP63alpha, using the same hypertrophic chondrocyte-specific Col10a1 control element. No skeletal abnormalities were detected in these Col10a1-DeltaNP63alpha transgenic mice at both E17.5 and P1 stages, suggesting less importance of DeltaNP63alpha during late embryonic skeletal development. To further investigate the function of P63 isoforms during early skeletal development, we have generated DeltaNP63alpha and TAP63alpha transgenic mice using a chondrocyte-specific Col2a1 control element. Surprisingly, while no skeletal defect was shown in the Col2a1-DeltaNP63alpha transgenic mice, reduced ossification was observed in the digit and tail bones of Col2a1-TAP63alpha transgenic mice at both E17.5 and P1 stages compared to their wild-type littermates. Expression profiling and immunohistochemical analysis detected upregulated expression of Sox9, a major negative regulator of endochondral ossification, in Col2a1-TAP63alpha transgenic mice. Taken together, our results suggest a distinct function of P63 isoforms, herein, DeltaNP63alpha and TAP63alpha, during endochondral ossification.
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