Literature DB >> 28472361

Energy Metabolism of the Osteoblast: Implications for Osteoporosis.

Wen-Chih Lee1, Anyonya R Guntur2, Fanxin Long1,3, Clifford J Rosen2.   

Abstract

Osteoblasts, the bone-forming cells of the remodeling unit, are essential for growth and maintenance of the skeleton. Clinical disorders of substrate availability (e.g., diabetes mellitus, anorexia nervosa, and aging) cause osteoblast dysfunction, ultimately leading to skeletal fragility and osteoporotic fractures. Conversely, anabolic treatments for osteoporosis enhance the work of the osteoblast by altering osteoblast metabolism. Emerging evidence supports glycolysis as the major metabolic pathway to meet ATP demand during osteoblast differentiation. Glut1 and Glut3 are the principal transporters of glucose in osteoblasts, although Glut4 has also been implicated. Wnt signaling induces osteoblast differentiation and activates glycolysis through mammalian target of rapamycin, whereas parathyroid hormone stimulates glycolysis through induction of insulin-like growth factor-I. Glutamine is an alternate fuel source for osteogenesis via the tricarboxylic acid cycle, and fatty acids can be metabolized to generate ATP via oxidative phosphorylation although temporal specificity has not been established. More studies with new model systems are needed to fully understand how the osteoblast utilizes fuel substrates in health and disease and how that impacts metabolic bone diseases.
Copyright © 2017 Endocrine Society.

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Year:  2017        PMID: 28472361      PMCID: PMC5460680          DOI: 10.1210/er.2017-00064

Source DB:  PubMed          Journal:  Endocr Rev        ISSN: 0163-769X            Impact factor:   19.871


  113 in total

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Authors:  W F Neuman; M W Neuman; R Brommage
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Authors:  Jianquan Chen; Xiaolin Tu; Emel Esen; Kyu Sang Joeng; Congxin Lin; Jeffrey M Arbeit; Markus A Rüegg; Michael N Hall; Liang Ma; Fanxin Long
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  100 in total

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Review 6.  Glucose metabolism in bone.

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7.  Loss of Nmp4 optimizes osteogenic metabolism and secretion to enhance bone quality.

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Journal:  Am J Physiol Endocrinol Metab       Date:  2019-01-15       Impact factor: 4.310

8.  Loss of P2X7 receptor function dampens whole body energy expenditure and fatty acid oxidation.

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10.  The Wnt pathway regulator expression levels and their relationship to bone metabolism in thoracolumbar osteoporotic vertebral compression fracture patients.

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