EP2 and EP4 receptors differentially mediate MAPK pathways underlying anabolic actions of prostaglandin E-2 on bone formation in rat calvaria cell cultures

Bone Volume 44 Issue 6 Page 1177-1185 published_at 2009-06
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Title ( eng )
EP2 and EP4 receptors differentially mediate MAPK pathways underlying anabolic actions of prostaglandin E-2 on bone formation in rat calvaria cell cultures
Creator
Aubin Jane E
Maeda Norihiko
Source Title
Bone
Volume 44
Issue 6
Start Page 1177
End Page 1185
Abstract
Of the four prostaglandin (PG) E receptor subtypes (EP1-EP4), EP2 and EP4 have been proposed to mediate the anabolic action of PGE(2) on bone formation but comparative evaluation Studies of EPs on bone formation do not necessarily share a common mechanism, implying that their additional features including downstream MAPK pathways may be beneficial to resolve this issue. We systematically assessed the roles of EPs in the rat calvaria (RC) cell Culture model by using four selective EP agonists (EPAs). Consistent with relative expression levels of the respective receptors, multiple phenotypic traits of bone formation in vitro, including proliferation of nodule-associated cells, osteoblast market expression and mineralized nodule formation were upregulated not only by PGE(2) but equally by EP2A and EP4A, but not by EP1A and EP3A. EP2A and EP4A were effective when cells were treated chronically or pulse-treated during nascent nodule formation. EP2A and EP4A equally stimulated the endogenous PGE(2) production, while EP2A caused a greater increase in cAMP production and c-Fos gene expression compared to EP4A. EP2A and EP4A activated predominantly p38 MAPK and ERK respectively, while c-Jun N-terminal kinase (JNK) was equally activated by both agonists. SB203580 (p38 MAPK inhibitor) blocked the PGE(2) effect on mineralized nodule formation, while U0126 (ERK inhibitor) and dicumarol (JNK inhibitor) were less effective. PGE(2)-dependent phosphorylation of the MAPKs was affected not only by protein kinase (PK)A and PKC inhibitors but also by adenylate cyclase and PKC activators. Co-treatment of RC cells with EP2A or EP4A and bone morphogenetic protein (BMP)2, whose effects on bone nodule formation is known to be, in part, mediated through the PKA and p38 MAPK pathways, resulted in an additive effect on mineralized nodule formation. Further, PGE2, EP2A and EP4A did not increase BMP2/4 mRNA levels in RC cells, and EP2-induced phosphorylation of p38 MAPK was not eliminated by Noggin. These results Suggest that, in the RC cell m
Keywords
Selective EP agonists
Rat calvaria cells
Osteoblastogenesis
MAPKs
Prostaglandin E
NDC
Medical sciences [ 490 ]
Language
eng
Resource Type journal article
Publisher
Elsevier Science Inc
Date of Issued 2009-06
Rights
Copyright (c) 2009 Elsevier Inc. All rights reserved.
Publish Type Author’s Original
Access Rights open access
Source Identifier
[ISSN] 8756-3282
[DOI] 10.1016/j.bone.2009.02.010
[NCID] AA10506985
[DOI] http://dx.doi.org/10.1016/j.bone.2009.02.010