Systems-based identification of temporal processing pathways during bone cell mechanotransduction.

Bone has long been established to be a highly mechanosensitive tissue. When subjected to mechanical loading, bone exhibits profoundly different anabolic responses depending on the temporal pattern in which the stimulus is applied. This phenomenon has been termed temporal processing, and involves com...

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Main Authors: Leah E Worton, Brandon J Ausk, Leah M Downey, Steven D Bain, Edith M Gardiner, Sundar Srinivasan, Ted S Gross, Ronald Y Kwon
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3770665?pdf=render
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spelling doaj-9c0c15401563429c86f952ae64e9efca2020-11-25T02:15:27ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0189e7420510.1371/journal.pone.0074205Systems-based identification of temporal processing pathways during bone cell mechanotransduction.Leah E WortonBrandon J AuskLeah M DowneySteven D BainEdith M GardinerSundar SrinivasanTed S GrossRonald Y KwonBone has long been established to be a highly mechanosensitive tissue. When subjected to mechanical loading, bone exhibits profoundly different anabolic responses depending on the temporal pattern in which the stimulus is applied. This phenomenon has been termed temporal processing, and involves complex signal amplification mechanisms that are largely unidentified. In this study, our goal was to characterize transcriptomic perturbations arising from the insertion of intermittent rest periods (a temporal variation with profound effects on bone anabolism) in osteoblastic cells subjected to fluid flow, and assess the utility of these perturbations to identify signaling pathways that are differentially activated by this temporal variation. At the level of the genome, we found that the common and differential alterations in gene expression arising from the two flow conditions were distributionally distinct, with the differential alterations characterized by many small changes in a large number of genes. Using bioinformatics analysis, we identified distinct up- and down-regulation transcriptomic signatures associated with the insertion of rest intervals, and found that the up-regulation signature was significantly associated with MAPK signaling. Confirming the involvement of the MAPK pathway, we found that the insertion of rest intervals significantly elevated flow-induced p-ERK1/2 levels by enabling a second spike in activity that was not observed in response to continuous flow. Collectively, these studies are the first to characterize distinct transcriptomic perturbations in bone cells subjected to continuous and intermittent stimulation, and directly demonstrate the utility of systems-based transcriptomic analysis to identify novel acute signaling pathways underlying temporal processing in bone cells.http://europepmc.org/articles/PMC3770665?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Leah E Worton
Brandon J Ausk
Leah M Downey
Steven D Bain
Edith M Gardiner
Sundar Srinivasan
Ted S Gross
Ronald Y Kwon
spellingShingle Leah E Worton
Brandon J Ausk
Leah M Downey
Steven D Bain
Edith M Gardiner
Sundar Srinivasan
Ted S Gross
Ronald Y Kwon
Systems-based identification of temporal processing pathways during bone cell mechanotransduction.
PLoS ONE
author_facet Leah E Worton
Brandon J Ausk
Leah M Downey
Steven D Bain
Edith M Gardiner
Sundar Srinivasan
Ted S Gross
Ronald Y Kwon
author_sort Leah E Worton
title Systems-based identification of temporal processing pathways during bone cell mechanotransduction.
title_short Systems-based identification of temporal processing pathways during bone cell mechanotransduction.
title_full Systems-based identification of temporal processing pathways during bone cell mechanotransduction.
title_fullStr Systems-based identification of temporal processing pathways during bone cell mechanotransduction.
title_full_unstemmed Systems-based identification of temporal processing pathways during bone cell mechanotransduction.
title_sort systems-based identification of temporal processing pathways during bone cell mechanotransduction.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Bone has long been established to be a highly mechanosensitive tissue. When subjected to mechanical loading, bone exhibits profoundly different anabolic responses depending on the temporal pattern in which the stimulus is applied. This phenomenon has been termed temporal processing, and involves complex signal amplification mechanisms that are largely unidentified. In this study, our goal was to characterize transcriptomic perturbations arising from the insertion of intermittent rest periods (a temporal variation with profound effects on bone anabolism) in osteoblastic cells subjected to fluid flow, and assess the utility of these perturbations to identify signaling pathways that are differentially activated by this temporal variation. At the level of the genome, we found that the common and differential alterations in gene expression arising from the two flow conditions were distributionally distinct, with the differential alterations characterized by many small changes in a large number of genes. Using bioinformatics analysis, we identified distinct up- and down-regulation transcriptomic signatures associated with the insertion of rest intervals, and found that the up-regulation signature was significantly associated with MAPK signaling. Confirming the involvement of the MAPK pathway, we found that the insertion of rest intervals significantly elevated flow-induced p-ERK1/2 levels by enabling a second spike in activity that was not observed in response to continuous flow. Collectively, these studies are the first to characterize distinct transcriptomic perturbations in bone cells subjected to continuous and intermittent stimulation, and directly demonstrate the utility of systems-based transcriptomic analysis to identify novel acute signaling pathways underlying temporal processing in bone cells.
url http://europepmc.org/articles/PMC3770665?pdf=render
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