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The Effect of Oxandrolone Treatment on Human Osteoblastic Cells

Objective: Oxandrolone, administered to severely burned children over the first year postburn, produces increased lean body mass by 6 months; however, an increase in total body bone mineral requires 12 months. Consequently, this bone mineral response may be due to increased muscle mass. Alternativel...

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Autores principales: Xiang Bi, Lian, M. Wiren, Kristine, Zhang, Xiao-Wei, V. Oliveira, Gisele, L. Klein, Gordon, G. Mainous, Elgene, N. Herndon, David
Formato: Texto
Lenguaje:English
Publicado: Open Science Company, LLC 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1828036/
https://www.ncbi.nlm.nih.gov/pubmed/17364004
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author Xiang Bi, Lian
M. Wiren, Kristine
Zhang, Xiao-Wei
V. Oliveira, Gisele
L. Klein, Gordon
G. Mainous, Elgene
N. Herndon, David
author_facet Xiang Bi, Lian
M. Wiren, Kristine
Zhang, Xiao-Wei
V. Oliveira, Gisele
L. Klein, Gordon
G. Mainous, Elgene
N. Herndon, David
author_sort Xiang Bi, Lian
collection PubMed
description Objective: Oxandrolone, administered to severely burned children over the first year postburn, produces increased lean body mass by 6 months; however, an increase in total body bone mineral requires 12 months. Consequently, this bone mineral response may be due to increased muscle mass. Alternatively, oxandrolone may act directly on bone. The current study seeks to determine whether oxandrolone can transactivate the androgen receptor in osteoblasts. Methods: Collagen, alkaline phosphatase, osteocalcin, osteoprotegerin, and androgen receptor abundance were determined by qRT-PCR, confocal laser scanning microscopy, or immunoquantitative assay. To determine the effect of oxandrolone on gene expression in differentiated cells, osteocytic cultures were grown to confluence in differentiation medium and then treated 24 hours or 5 days with 15 μg/mL oxandrolone. Results: Increased nuclear fluorescence of the androgen receptor and increased cellular type I collagen were observed with oxandrolone at 15 and 30 μg/mL but not at lower doses. Alkaline phosphatase (7%–20%) and osteocalcin (13%–18%) increases were modest but significant. Short-term treatment produced no significant effects, but at 5 days androgen receptor levels were increased while collagen levels were significantly decreased, with little effect on alkaline phosphatase, osteocalcin, or osteoprotegerin. Conclusions: These data suggest oxandrolone can stimulate production of osteoblast differentiation markers in proliferating osteoblastic cells, most likely through the androgen receptor; however, with longer treatment in mature cells, oxandrolone decreases collagen expression. Thus it is possible that oxandrolone given to burned children acts directly on immature osteoblasts to stimulate collagen production, but also may have positive effects to increase bone mineral through other mechanisms.
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spelling pubmed-18280362007-04-10 The Effect of Oxandrolone Treatment on Human Osteoblastic Cells Xiang Bi, Lian M. Wiren, Kristine Zhang, Xiao-Wei V. Oliveira, Gisele L. Klein, Gordon G. Mainous, Elgene N. Herndon, David J Burns Wounds Article Objective: Oxandrolone, administered to severely burned children over the first year postburn, produces increased lean body mass by 6 months; however, an increase in total body bone mineral requires 12 months. Consequently, this bone mineral response may be due to increased muscle mass. Alternatively, oxandrolone may act directly on bone. The current study seeks to determine whether oxandrolone can transactivate the androgen receptor in osteoblasts. Methods: Collagen, alkaline phosphatase, osteocalcin, osteoprotegerin, and androgen receptor abundance were determined by qRT-PCR, confocal laser scanning microscopy, or immunoquantitative assay. To determine the effect of oxandrolone on gene expression in differentiated cells, osteocytic cultures were grown to confluence in differentiation medium and then treated 24 hours or 5 days with 15 μg/mL oxandrolone. Results: Increased nuclear fluorescence of the androgen receptor and increased cellular type I collagen were observed with oxandrolone at 15 and 30 μg/mL but not at lower doses. Alkaline phosphatase (7%–20%) and osteocalcin (13%–18%) increases were modest but significant. Short-term treatment produced no significant effects, but at 5 days androgen receptor levels were increased while collagen levels were significantly decreased, with little effect on alkaline phosphatase, osteocalcin, or osteoprotegerin. Conclusions: These data suggest oxandrolone can stimulate production of osteoblast differentiation markers in proliferating osteoblastic cells, most likely through the androgen receptor; however, with longer treatment in mature cells, oxandrolone decreases collagen expression. Thus it is possible that oxandrolone given to burned children acts directly on immature osteoblasts to stimulate collagen production, but also may have positive effects to increase bone mineral through other mechanisms. Open Science Company, LLC 2007-03-07 /pmc/articles/PMC1828036/ /pubmed/17364004 Text en Copyright © 2007 The Author(s) http://creativecommons.org/licenses/by/2.0/ This is an open-access article whereby the authors retain copyright of the work. The article is distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Article
Xiang Bi, Lian
M. Wiren, Kristine
Zhang, Xiao-Wei
V. Oliveira, Gisele
L. Klein, Gordon
G. Mainous, Elgene
N. Herndon, David
The Effect of Oxandrolone Treatment on Human Osteoblastic Cells
title The Effect of Oxandrolone Treatment on Human Osteoblastic Cells
title_full The Effect of Oxandrolone Treatment on Human Osteoblastic Cells
title_fullStr The Effect of Oxandrolone Treatment on Human Osteoblastic Cells
title_full_unstemmed The Effect of Oxandrolone Treatment on Human Osteoblastic Cells
title_short The Effect of Oxandrolone Treatment on Human Osteoblastic Cells
title_sort effect of oxandrolone treatment on human osteoblastic cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1828036/
https://www.ncbi.nlm.nih.gov/pubmed/17364004
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