Insulin Signaling in Osteoblasts Integrates Bone Remodeling and Energy Metabolism

Mathieu Ferron; Jianwen Wei; Tatsuya Yoshizawa; Andrea Del Fattore; Ronald A. DePinho; Anna Teti; Patricia Ducy; Gerard Karsenty

doi:10.1016/j.cell.2010.06.003

Insulin Signaling in Osteoblasts Integrates Bone Remodeling and Energy Metabolism

Mathieu Ferron, Jianwen Wei, Tatsuya Yoshizawa, Andrea Del Fattore, Ronald A. DePinho, Anna Teti, Patricia Ducy, Gerard Karsenty

Research output: Contribution to journal › Article › peer-review

904 Scopus citations

Abstract

The broad expression of the insulin receptor suggests that the spectrum of insulin function has not been fully described. A cell type expressing this receptor is the osteoblast, a bone-specific cell favoring glucose metabolism through a hormone, osteocalcin, that becomes active once uncarboxylated. We show here that insulin signaling in osteoblasts is necessary for whole-body glucose homeostasis because it increases osteocalcin activity. To achieve this function insulin signaling in osteoblasts takes advantage of the regulation of osteoclastic bone resorption exerted by osteoblasts. Indeed, since bone resorption occurs at a pH acidic enough to decarboxylate proteins, osteoclasts determine the carboxylation status and function of osteocalcin. Accordingly, increasing or decreasing insulin signaling in osteoblasts promotes or hampers glucose metabolism in a bone resorption-dependent manner in mice and humans. Hence, in a feed-forward loop, insulin signals in osteoblasts activate a hormone, osteocalcin, that promotes glucose metabolism.

Original language	English (US)
Pages (from-to)	296-308
Number of pages	13
Journal	Cell
Volume	142
Issue number	2
DOIs	https://doi.org/10.1016/j.cell.2010.06.003
State	Published - Jul 2010
Externally published	Yes

Keywords

Humdisease
Signaling

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

Access to Document

10.1016/j.cell.2010.06.003

Cite this

@article{9202323c41904a8c940bc3f0ba59698b,

title = "Insulin Signaling in Osteoblasts Integrates Bone Remodeling and Energy Metabolism",

abstract = "The broad expression of the insulin receptor suggests that the spectrum of insulin function has not been fully described. A cell type expressing this receptor is the osteoblast, a bone-specific cell favoring glucose metabolism through a hormone, osteocalcin, that becomes active once uncarboxylated. We show here that insulin signaling in osteoblasts is necessary for whole-body glucose homeostasis because it increases osteocalcin activity. To achieve this function insulin signaling in osteoblasts takes advantage of the regulation of osteoclastic bone resorption exerted by osteoblasts. Indeed, since bone resorption occurs at a pH acidic enough to decarboxylate proteins, osteoclasts determine the carboxylation status and function of osteocalcin. Accordingly, increasing or decreasing insulin signaling in osteoblasts promotes or hampers glucose metabolism in a bone resorption-dependent manner in mice and humans. Hence, in a feed-forward loop, insulin signals in osteoblasts activate a hormone, osteocalcin, that promotes glucose metabolism.",

keywords = "Humdisease, Signaling",

author = "Mathieu Ferron and Jianwen Wei and Tatsuya Yoshizawa and {Del Fattore}, Andrea and DePinho, {Ronald A.} and Anna Teti and Patricia Ducy and Gerard Karsenty",

note = "Funding Information: We thank Drs. S. Kousteni, T. Zee, R.L. Levine, M. Tremblay, and J. Vacher for reagents; Dr. J. Lacombe for help with transplantations; Drs. K. Henriksen and J. Bollerslev for generously sharing patient serum samples; Dr. T. Lam at the W.M. Keck Foundation Biotechnology Resource Laboratory, Yale University, for FT-ICR mass spectral analyses; and Drs. J.K. Kim and F. Mauvais-Jarvis for critical reading of the manuscript. This work was supported by a fellowship from the Fond de la recherche en sant{\'e} du Qu{\'e}bec (M.F.), grants from the National Institutes of Health (G.K.), and the Juvenile Diabetes Research Foundation (P.D.). G.K. is a founder and member of the scientific advisory board of Escoublac Inc. P.D. is a founder and consultant of Escoublac Inc. ",

year = "2010",

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doi = "10.1016/j.cell.2010.06.003",

language = "English (US)",

volume = "142",

pages = "296--308",

journal = "Cell",

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T1 - Insulin Signaling in Osteoblasts Integrates Bone Remodeling and Energy Metabolism

AU - Ferron, Mathieu

AU - Wei, Jianwen

AU - Yoshizawa, Tatsuya

AU - Del Fattore, Andrea

AU - DePinho, Ronald A.

AU - Teti, Anna

AU - Ducy, Patricia

AU - Karsenty, Gerard

N1 - Funding Information: We thank Drs. S. Kousteni, T. Zee, R.L. Levine, M. Tremblay, and J. Vacher for reagents; Dr. J. Lacombe for help with transplantations; Drs. K. Henriksen and J. Bollerslev for generously sharing patient serum samples; Dr. T. Lam at the W.M. Keck Foundation Biotechnology Resource Laboratory, Yale University, for FT-ICR mass spectral analyses; and Drs. J.K. Kim and F. Mauvais-Jarvis for critical reading of the manuscript. This work was supported by a fellowship from the Fond de la recherche en santé du Québec (M.F.), grants from the National Institutes of Health (G.K.), and the Juvenile Diabetes Research Foundation (P.D.). G.K. is a founder and member of the scientific advisory board of Escoublac Inc. P.D. is a founder and consultant of Escoublac Inc.

PY - 2010/7

Y1 - 2010/7

N2 - The broad expression of the insulin receptor suggests that the spectrum of insulin function has not been fully described. A cell type expressing this receptor is the osteoblast, a bone-specific cell favoring glucose metabolism through a hormone, osteocalcin, that becomes active once uncarboxylated. We show here that insulin signaling in osteoblasts is necessary for whole-body glucose homeostasis because it increases osteocalcin activity. To achieve this function insulin signaling in osteoblasts takes advantage of the regulation of osteoclastic bone resorption exerted by osteoblasts. Indeed, since bone resorption occurs at a pH acidic enough to decarboxylate proteins, osteoclasts determine the carboxylation status and function of osteocalcin. Accordingly, increasing or decreasing insulin signaling in osteoblasts promotes or hampers glucose metabolism in a bone resorption-dependent manner in mice and humans. Hence, in a feed-forward loop, insulin signals in osteoblasts activate a hormone, osteocalcin, that promotes glucose metabolism.

AB - The broad expression of the insulin receptor suggests that the spectrum of insulin function has not been fully described. A cell type expressing this receptor is the osteoblast, a bone-specific cell favoring glucose metabolism through a hormone, osteocalcin, that becomes active once uncarboxylated. We show here that insulin signaling in osteoblasts is necessary for whole-body glucose homeostasis because it increases osteocalcin activity. To achieve this function insulin signaling in osteoblasts takes advantage of the regulation of osteoclastic bone resorption exerted by osteoblasts. Indeed, since bone resorption occurs at a pH acidic enough to decarboxylate proteins, osteoclasts determine the carboxylation status and function of osteocalcin. Accordingly, increasing or decreasing insulin signaling in osteoblasts promotes or hampers glucose metabolism in a bone resorption-dependent manner in mice and humans. Hence, in a feed-forward loop, insulin signals in osteoblasts activate a hormone, osteocalcin, that promotes glucose metabolism.

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Insulin Signaling in Osteoblasts Integrates Bone Remodeling and Energy Metabolism

Abstract

Keywords

ASJC Scopus subject areas

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