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   Dual effects of heparin on BMP-2-induced osteogenic activity in MC3T3-E1 cells  
   
نویسنده kanzaki s. ,ariyoshi w. ,takahashi t. ,okinaga t. ,kaneuji t. ,mitsugi s. ,nakashima k. ,tsujisawa t. ,nishihara t.
منبع pharmacological reports - 2011 - دوره : 63 - شماره : 5 - صفحه:1222 -1230
چکیده    Heparin displays several types of biological activities by binding to various extracellular molecules,including pivotal roles in bone metabolism. we have previously reported that heparin competitively inhibits the binding activity of bone morphogenic protein-2 (bmp-2) to bmp and the bmp receptor (bmpr) and suppresses bmp-2 osteogenic activity. in the present study,we examined whether heparin affects osteoblast differentiation induced by bmp-2 at various time points in vitro. we found that 72 h of treatment with heparin inhibited alkaline phosphatase (alp) activity. however,144 h of treatment enhanced the alp activity in bmp-2-stimulated mc3t3-e1 cells. although heparin decreased the phosphorylation of smad1/5/8 after 0.5 h of culture,prolonged periods of culture with heparin enhanced the smad phosphorylation. in addition,72 h of treatment with heparin enhanced the mrna expression of runx2 and osterix in bmp-2-stimulated mc3t3-e1 cells. furthermore,them rna expression of bmp antagonists and inhibitory smads induced by bmp-2 was preferentially blocked by heparin at the 24 and 48 h time points. these findings indicate biphasic effects of heparin on bmp-2 activity and suggest that heparin has complex effects on the bmp-2 osteogenic bioactivities. prolonged culture with heparin stimulated bmp-2-induced osteogenic activity via down-regulation of bmp-2 antagonists and inhibitory smads. copyright © 2011 by institute of pharmacology polish academy of sciences.
کلیدواژه BMP-2; Heparin; Osteoblast; Osterix; Runx2; Smad
آدرس division of infections and molecular biology,department of health promotion,kyushu dental college,kitakyushu 803-8580,japan,division of oral and maxillofacial reconstructive surgery,department of oral and maxillofacial surgery,kyushu dental college,kitakyushu 803-8580, Japan, division of infections and molecular biology,department of health promotion,kyushu dental college,kitakyushu 803-8580, Japan, division of oral and maxillofacial reconstructive surgery,department of oral and maxillofacial surgery,kyushu dental college,kitakyushu 803-8580, Japan, division of infections and molecular biology,department of health promotion,kyushu dental college,kitakyushu 803-8580, Japan, division of infections and molecular biology,department of health promotion,kyushu dental college,kitakyushu 803-8580,japan,division of oral and maxillofacial reconstructive surgery,department of oral and maxillofacial surgery,kyushu dental college,kitakyushu 803-8580, Japan, division of infections and molecular biology,department of health promotion,kyushu dental college,kitakyushu 803-8580,japan,division of oral and maxillofacial reconstructive surgery,department of oral and maxillofacial surgery,kyushu dental college,kitakyushu 803-8580, Japan, division of periodontology,department of cariology and periodontology,kyushu dental college,kitakyushu 803-8580, Japan, department of oral health management,school of oral health sciences,kyushu dental college,kitakyushu 803-8580, Japan, division of infections and molecular biology,department of health promotion,kyushu dental college,kitakyushu 803-8580, Japan
 
     
   
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