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A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth

Citrate is a critical metabolic substrate and key regulator of energy metabolism in mammalian cells. It has been known for decades that the skeleton contains most (>85%) of the body’s citrate, but the question of why and how this metabolite should be partitioned in bone has received singularly li...

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Autores principales: Dirckx, Naomi, Zhang, Qian, Chu, Emily Y., Tower, Robert J., Li, Zhu, Guo, Shenghao, Yuan, Shichen, Khare, Pratik A., Zhang, Cissy, Verardo, Angela, Alejandro, Lucy O., Park, Angelina, Faugere, Marie-Claude, Helfand, Stephen L., Somerman, Martha J., Riddle, Ryan C., de Cabo, Rafael, Le, Anne, Schmidt-Rohr, Klaus, Clemens, Thomas L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: National Academy of Sciences 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9659386/
https://www.ncbi.nlm.nih.gov/pubmed/36322718
http://dx.doi.org/10.1073/pnas.2212178119
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author Dirckx, Naomi
Zhang, Qian
Chu, Emily Y.
Tower, Robert J.
Li, Zhu
Guo, Shenghao
Yuan, Shichen
Khare, Pratik A.
Zhang, Cissy
Verardo, Angela
Alejandro, Lucy O.
Park, Angelina
Faugere, Marie-Claude
Helfand, Stephen L.
Somerman, Martha J.
Riddle, Ryan C.
de Cabo, Rafael
Le, Anne
Schmidt-Rohr, Klaus
Clemens, Thomas L.
author_facet Dirckx, Naomi
Zhang, Qian
Chu, Emily Y.
Tower, Robert J.
Li, Zhu
Guo, Shenghao
Yuan, Shichen
Khare, Pratik A.
Zhang, Cissy
Verardo, Angela
Alejandro, Lucy O.
Park, Angelina
Faugere, Marie-Claude
Helfand, Stephen L.
Somerman, Martha J.
Riddle, Ryan C.
de Cabo, Rafael
Le, Anne
Schmidt-Rohr, Klaus
Clemens, Thomas L.
author_sort Dirckx, Naomi
collection PubMed
description Citrate is a critical metabolic substrate and key regulator of energy metabolism in mammalian cells. It has been known for decades that the skeleton contains most (>85%) of the body’s citrate, but the question of why and how this metabolite should be partitioned in bone has received singularly little attention. Here, we show that osteoblasts use a specialized metabolic pathway to regulate uptake, endogenous production, and the deposition of citrate into bone. Osteoblasts express high levels of the membranous Na(+)-dependent citrate transporter solute carrier family 13 member 5 (Slc13a5) gene. Inhibition or genetic disruption of Slc13a5 reduced osteogenic citrate uptake and disrupted mineral nodule formation. Bones from mice lacking Slc13a5 globally, or selectively in osteoblasts, showed equivalent reductions in cortical thickness, with similarly compromised mechanical strength. Surprisingly, citrate content in mineral from Slc13a5(−/−) osteoblasts was increased fourfold relative to controls, suggesting the engagement of compensatory mechanisms to augment endogenous citrate production. Indeed, through the coordinated functioning of the apical membrane citrate transporter SLC13A5 and a mitochondrial zinc transporter protein (ZIP1; encoded by Slc39a1), a mediator of citrate efflux from the tricarboxylic acid cycle, SLC13A5 mediates citrate entry from blood and its activity exerts homeostatic control of cytoplasmic citrate. Intriguingly, Slc13a5-deficient mice also exhibited defective tooth enamel and dentin formation, a clinical feature, which we show is recapitulated in primary teeth from children with SLC13A5 mutations. Together, our results reveal the components of an osteoblast metabolic pathway, which affects bone strength by regulating citrate deposition into mineral hydroxyapatite.
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spelling pubmed-96593862023-05-02 A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth Dirckx, Naomi Zhang, Qian Chu, Emily Y. Tower, Robert J. Li, Zhu Guo, Shenghao Yuan, Shichen Khare, Pratik A. Zhang, Cissy Verardo, Angela Alejandro, Lucy O. Park, Angelina Faugere, Marie-Claude Helfand, Stephen L. Somerman, Martha J. Riddle, Ryan C. de Cabo, Rafael Le, Anne Schmidt-Rohr, Klaus Clemens, Thomas L. Proc Natl Acad Sci U S A Biological Sciences Citrate is a critical metabolic substrate and key regulator of energy metabolism in mammalian cells. It has been known for decades that the skeleton contains most (>85%) of the body’s citrate, but the question of why and how this metabolite should be partitioned in bone has received singularly little attention. Here, we show that osteoblasts use a specialized metabolic pathway to regulate uptake, endogenous production, and the deposition of citrate into bone. Osteoblasts express high levels of the membranous Na(+)-dependent citrate transporter solute carrier family 13 member 5 (Slc13a5) gene. Inhibition or genetic disruption of Slc13a5 reduced osteogenic citrate uptake and disrupted mineral nodule formation. Bones from mice lacking Slc13a5 globally, or selectively in osteoblasts, showed equivalent reductions in cortical thickness, with similarly compromised mechanical strength. Surprisingly, citrate content in mineral from Slc13a5(−/−) osteoblasts was increased fourfold relative to controls, suggesting the engagement of compensatory mechanisms to augment endogenous citrate production. Indeed, through the coordinated functioning of the apical membrane citrate transporter SLC13A5 and a mitochondrial zinc transporter protein (ZIP1; encoded by Slc39a1), a mediator of citrate efflux from the tricarboxylic acid cycle, SLC13A5 mediates citrate entry from blood and its activity exerts homeostatic control of cytoplasmic citrate. Intriguingly, Slc13a5-deficient mice also exhibited defective tooth enamel and dentin formation, a clinical feature, which we show is recapitulated in primary teeth from children with SLC13A5 mutations. Together, our results reveal the components of an osteoblast metabolic pathway, which affects bone strength by regulating citrate deposition into mineral hydroxyapatite. National Academy of Sciences 2022-11-02 2022-11-08 /pmc/articles/PMC9659386/ /pubmed/36322718 http://dx.doi.org/10.1073/pnas.2212178119 Text en Copyright © 2022 the Author(s). Published by PNAS. https://creativecommons.org/licenses/by-nc-nd/4.0/This article is distributed under Creative Commons Attribution-NonCommercial-NoDerivatives License 4.0 (CC BY-NC-ND) (https://creativecommons.org/licenses/by-nc-nd/4.0/) .
spellingShingle Biological Sciences
Dirckx, Naomi
Zhang, Qian
Chu, Emily Y.
Tower, Robert J.
Li, Zhu
Guo, Shenghao
Yuan, Shichen
Khare, Pratik A.
Zhang, Cissy
Verardo, Angela
Alejandro, Lucy O.
Park, Angelina
Faugere, Marie-Claude
Helfand, Stephen L.
Somerman, Martha J.
Riddle, Ryan C.
de Cabo, Rafael
Le, Anne
Schmidt-Rohr, Klaus
Clemens, Thomas L.
A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
title A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
title_full A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
title_fullStr A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
title_full_unstemmed A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
title_short A specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
title_sort specialized metabolic pathway partitions citrate in hydroxyapatite to impact mineralization of bones and teeth
topic Biological Sciences
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9659386/
https://www.ncbi.nlm.nih.gov/pubmed/36322718
http://dx.doi.org/10.1073/pnas.2212178119
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