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Published October 17, 2017 | Published
Journal Article Open

Targeted Pth4-expressing cell ablation impairs skeletal mineralization in zebrafish

Abstract

Skeletal development and mineralization are essential processes driven by the coordinated action of neural signals, circulating molecules and local factors. Our previous studies revealed that the novel neuropeptide Pth4, synthesized by hypothalamic cells, was involved in bone metabolism via phosphate regulation in adult zebrafish. Here, we investigate the role of pth4 during skeletal development using single-cell resolution, two-photon laser ablation of Pth4:eGFP-expressing cells and confocal imaging in vivo. Using a stable transgenic Pth4:eGFP zebrafish line, we identify Pth4:eGFP-expressing cells as post-mitotic neurons. After targeted ablation of eGFP-expressing cells in the hypothalamus, the experimental larvae exhibited impaired mineralization of the craniofacial bones whereas cartilage development was normal. In addition to a decrease in pth4 transcript levels, we noted altered expression of phex and entpd5, genes associated with phosphate homeostasis and mineralization, as well as a delay in the expression of osteoblast differentiation markers such as sp7 and sparc. Taken together, these results suggest that Pth4-expressing hypothalamic neurons participate in the regulation of bone metabolism, possibly through regulating phosphate balance during zebrafish development.

Additional Information

© 2017 Suarez-Bregua et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Received: June 1, 2017; Accepted: October 2, 2017; Published: October 17, 2017. Data Availability Statement: All relevant data are within the paper. This work was funded by the Spanish Economy and Competitiveness Ministry project ALG2011-23581 and AGL2014-52473R to JR. AS was supported by a National Institutes of Health (NIH) grant R01DE024157 and PSB was supported by a Campus do Mar PhD grant, Xunta de Galicia (PRE/2012/532) and AGL2014-52473R project contract. The authors have declared that no competing interests exist. Author Contributions: Formal analysis: Paula Suarez-Bregua. Funding acquisition: Josep Rotllant. Investigation: Paula Suarez-Bregua, Ankur Saxena, Marianne E. Bronner, Josep Rotllant. Methodology: Paula Suarez-Bregua, Ankur Saxena. Project administration: Marianne E. Bronner, Josep Rotllant. Supervision: Ankur Saxena, Marianne E. Bronner, Josep Rotllant. Writing ± original draft: Paula Suarez-Bregua. Writing ± review & editing: Ankur Saxena, Marianne E. Bronner, Josep Rotllant.

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Created:
August 19, 2023
Modified:
October 17, 2023