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More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish

Dietary phosphorus (P) is essential for bone mineralisation in vertebrates. P deficiency can cause growth retardation, osteomalacia and bone deformities, both in teleosts and in mammals. Conversely, excess P supply can trigger soft tissue calcification and bone hypermineralisation. This study uses a...

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Autores principales: Cotti, Silvia, Huysseune, Ann, Koppe, Wolfgang, Rücklin, Martin, Marone, Federica, Wölfel, Eva M., Fiedler, Imke A. K., Busse, Björn, Forlino, Antonella, Witten, P. Eckhard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7432380/
https://www.ncbi.nlm.nih.gov/pubmed/32751494
http://dx.doi.org/10.3390/ijms21155429
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author Cotti, Silvia
Huysseune, Ann
Koppe, Wolfgang
Rücklin, Martin
Marone, Federica
Wölfel, Eva M.
Fiedler, Imke A. K.
Busse, Björn
Forlino, Antonella
Witten, P. Eckhard
author_facet Cotti, Silvia
Huysseune, Ann
Koppe, Wolfgang
Rücklin, Martin
Marone, Federica
Wölfel, Eva M.
Fiedler, Imke A. K.
Busse, Björn
Forlino, Antonella
Witten, P. Eckhard
author_sort Cotti, Silvia
collection PubMed
description Dietary phosphorus (P) is essential for bone mineralisation in vertebrates. P deficiency can cause growth retardation, osteomalacia and bone deformities, both in teleosts and in mammals. Conversely, excess P supply can trigger soft tissue calcification and bone hypermineralisation. This study uses a wide range of complementary techniques (X-rays, histology, TEM, synchrotron X-ray tomographic microscopy, nanoindentation) to describe in detail the effects of dietary P on the zebrafish skeleton, after two months of administering three different diets: 0.5% (low P, LP), 1.0% (regular P, RP), and 1.5% (high P, HP) total P content. LP zebrafish display growth retardation and hypomineralised bones, albeit without deformities. LP zebrafish increase production of non-mineralised bone matrix, and osteoblasts have enlarged endoplasmic reticulum cisternae, indicative for increased collagen synthesis. The HP diet promotes growth, high mineralisation, and stiffness but causes vertebral centra fusions. Structure and arrangement of bone matrix collagen fibres are not influenced by dietary P in all three groups. In conclusion, low dietary P content stimulates the formation of non-mineralised bone without inducing malformations. This indicates that bone formation and mineralisation are uncoupled. In contrast, high dietary P content promotes mineralisation and vertebral body fusions. This new zebrafish model is a useful tool to understand the mechanisms underlying osteomalacia and abnormal mineralisation, due to underlying variations in dietary P levels.
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spelling pubmed-74323802020-08-24 More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish Cotti, Silvia Huysseune, Ann Koppe, Wolfgang Rücklin, Martin Marone, Federica Wölfel, Eva M. Fiedler, Imke A. K. Busse, Björn Forlino, Antonella Witten, P. Eckhard Int J Mol Sci Article Dietary phosphorus (P) is essential for bone mineralisation in vertebrates. P deficiency can cause growth retardation, osteomalacia and bone deformities, both in teleosts and in mammals. Conversely, excess P supply can trigger soft tissue calcification and bone hypermineralisation. This study uses a wide range of complementary techniques (X-rays, histology, TEM, synchrotron X-ray tomographic microscopy, nanoindentation) to describe in detail the effects of dietary P on the zebrafish skeleton, after two months of administering three different diets: 0.5% (low P, LP), 1.0% (regular P, RP), and 1.5% (high P, HP) total P content. LP zebrafish display growth retardation and hypomineralised bones, albeit without deformities. LP zebrafish increase production of non-mineralised bone matrix, and osteoblasts have enlarged endoplasmic reticulum cisternae, indicative for increased collagen synthesis. The HP diet promotes growth, high mineralisation, and stiffness but causes vertebral centra fusions. Structure and arrangement of bone matrix collagen fibres are not influenced by dietary P in all three groups. In conclusion, low dietary P content stimulates the formation of non-mineralised bone without inducing malformations. This indicates that bone formation and mineralisation are uncoupled. In contrast, high dietary P content promotes mineralisation and vertebral body fusions. This new zebrafish model is a useful tool to understand the mechanisms underlying osteomalacia and abnormal mineralisation, due to underlying variations in dietary P levels. MDPI 2020-07-30 /pmc/articles/PMC7432380/ /pubmed/32751494 http://dx.doi.org/10.3390/ijms21155429 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Cotti, Silvia
Huysseune, Ann
Koppe, Wolfgang
Rücklin, Martin
Marone, Federica
Wölfel, Eva M.
Fiedler, Imke A. K.
Busse, Björn
Forlino, Antonella
Witten, P. Eckhard
More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish
title More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish
title_full More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish
title_fullStr More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish
title_full_unstemmed More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish
title_short More Bone with Less Minerals? The Effects of Dietary Phosphorus on the Post-Cranial Skeleton in Zebrafish
title_sort more bone with less minerals? the effects of dietary phosphorus on the post-cranial skeleton in zebrafish
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7432380/
https://www.ncbi.nlm.nih.gov/pubmed/32751494
http://dx.doi.org/10.3390/ijms21155429
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