| Literature DB >> 26475502 |
Nobutaka Sato1, Jiro Ichikawa1, Masanori Wako1, Tetsuro Ohba1, Masanori Saito1, Hironao Sato1, Kensuke Koyama1, Tetsuo Hagino2, Jonathan G Schoenecker3, Takashi Ando4, Hirotaka Haro1.
Abstract
Thrombin (coagulation factor IIa) is a serine protease encoded by the F2 gene. Pro-thrombin (coagulation factor II) is cut to generate thrombin in the coagulation cascade that results in a reduction of blood loss. Procoagulant states that lead to activation of thrombin are common in bone fracture sites. However, its physiological roles and relationship with osteoblasts in bone fractures are largely unknown. We herein report various effects of thrombin on mouse osteoblastic MC3T3-E1 cells. MC3T3-E1 cells expressed proteinase-activated receptor 1 (PAR1), also known as the coagulation factor II receptor. They also produced monocyte chemoattractant protein (MCP-1), tissue factor (TF), MCSF and IL-6 upon thrombin stimulation through the PI3K-Akt and MEK-Erk1/2 pathways. Furthermore, MCP-1 obtained from thrombin-stimulated MC3T3-E1 cells induced migration by macrophage RAW264 cells. All these effects of thrombin on MC3T3-E1 cells were abolished by the selective non-peptide thrombin receptor inhibitor SCH79797. We also found that thrombin, PAR-1, MCP-1, TF as well as phosphorylated AKT and p42/44 were significantly expressed at the fracture site of mouse femoral bone. Collectively, thrombin/PAR-1 interaction regulated MCP-1, TF, MCSF and IL-6 production by MC3T3-E1 cells. Furthermore, MCP-1 induced RAW264 cell migration. Thrombin may thus be a novel cytokine that regulates several aspects of osteoblast function and fracture healing.Entities:
Keywords: Fracture model; MCP-1; Migration; PAR-1; Thrombin
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Year: 2015 PMID: 26475502 DOI: 10.1016/j.bone.2015.10.005
Source DB: PubMed Journal: Bone ISSN: 1873-2763 Impact factor: 4.398