NPPB and ACAN, two novel SHOX2 transcription targets implicated in skeletal development

Aza-Carmona, Miriam; Barca Tierno, Verónica; Hisado Oliva, Alberta; Belinchón, Alberta; Gorbenko del Blanco, Darya; Rodriguez, José Ignacio; Benito Sanz, Sara; Campos Barros, Ángel; Heath, Karen E.

Please use this identifier to cite or link to this item: http://hdl.handle.net/2445/118928

Title:	NPPB and ACAN, two novel SHOX2 transcription targets implicated in skeletal development
Author:	Aza-Carmona, Miriam Barca Tierno, Verónica Hisado Oliva, Alberta Belinchón, Alberta Gorbenko del Blanco, Darya Rodriguez, José Ignacio Benito Sanz, Sara Campos Barros, Ángel Heath, Karen E.
Keywords:	Factors de transcripció Transcripció genètica Malalties dels ossos Creixement dels ossos Transcription factors Genetic transcription Bone diseases Bones growth
Issue Date:	8-Jan-2014
Publisher:	Public Library of Science (PLoS)
Abstract:	SHOX and SHOX2 transcription factors are highly homologous, with even identical homeodomains. Genetic alterations in SHOX result in two skeletal dysplasias; Léri-Weill dyschondrosteosis (LWD) and Langer mesomelic dysplasia (LMD), while no human genetic disease has been linked to date with SHOX2. SHOX2 is, though, involved in skeletal development, as shown by different knockout mice models. Due to the high homology between SHOX and SHOX2, and their functional redundancy during heart development, we postulated that SHOX2 might have the same transcriptional targets and cofactors as SHOX in limb development. We selected two SHOX transcription targets regulated by different mechanisms: 1) the natriuretic peptide precursor B gene (NPPB) involved in the endochondral ossification signalling and directly activated by SHOX; and 2) Aggrecan (ACAN), a major component of cartilage extracellular matrix, regulated by the cooperation of SHOX with the SOX trio (SOX5, SOX6 and SOX9) via the protein interaction between SOX5/SOX6 and SHOX. Using the luciferase assay we have demonstrated that SHOX2, like SHOX, regulates NPPB directly whilst activates ACAN via its cooperation with the SOX trio. Subsequently, we have identified and characterized the protein domains implicated in the SHOX2 dimerization and also its protein interaction with SOX5/SOX6 and SHOX using the yeast-two hybrid and co-immunoprecipitation assays. Immunohistochemistry of human fetal growth plates from different time points demonstrated that SHOX2 is coexpressed with SHOX and the members of the SOX trio. Despite these findings, no mutation was identified in SHOX2 in a cohort of 83 LWD patients with no known molecular defect, suggesting that SHOX2 alterations do not cause LWD. In conclusion, our work has identified the first cofactors and two new transcription targets of SHOX2 in limb development, and we hypothesize a time- and tissue-specific functional redundancy between SHOX and SHOX2.
Note:	Reproducció del document publicat a: https://doi.org/10.1371/journal.pone.0083104
It is part of:	PLoS One, 2014, vol. 9, num. 1, p. e83104
URI:	http://hdl.handle.net/2445/118928
Related resource:	https://doi.org/10.1371/journal.pone.0083104
ISSN:	1932-6203
Appears in Collections:	Articles publicats en revistes (Biomedicina)

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