首页> 外文会议>Micro-NanoMechatronics and Human Science,MHS, 2008 International Symposium on >Loading of Mechanical Stress to Osteoblasts May Induce Cytokine Cross Talks between Osteoblasts and Monocytes/Macrophages in a JNK/p38-dependent Manner
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Loading of Mechanical Stress to Osteoblasts May Induce Cytokine Cross Talks between Osteoblasts and Monocytes/Macrophages in a JNK/p38-dependent Manner

机译:机械应力加载到成骨细胞上可能会导致成骨细胞与单核细胞/巨噬细胞以JNK / p38依赖的方式进行细胞因子串扰。

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Although mechanical stress has been shown to regulate bone modeling and remodeling, the mechanisms of bone remodeling after mechanical stress loading are not fully understood. We previously investigated the effects of loading of cyclic mechanical stretch on the activaties of JNK and p38 in MC3T3-E1 osteoblastic cells, and observed that JNK and p38 were activated by the mechanical stress. The patterns of their activation differed depending on the magnitude and duration of mechanical stress. In this study, we performed DNA microarray and quantitative RT-PCR analyses to investigate the biological outputs induced by activation of JNK and p38. We observed that expression of a number of genes was induced by mechanical stress-ehnanced activation of JNK and p38. One of these genes was osteoprotegerin which is a major bone metabolism related gene. The list of the genes also included Fn14monocyte, a cytokine receptor family member whose ligand had been known to be produced by monocytes and macrophages, and monocyte chemoattractant protein-3. These data suggests that mechanical stress-activated JNK and p38 induce cytokine cross talks between osteoblasts and bone marrow-derived monocytes and macrophages, which may play key roles in bone remodeling.
机译:尽管已经显示出机械应力可以调节骨骼的建模和重塑,但是对机械应力加载后骨骼重塑的机制还没有完全了解。我们先前研究了循环机械拉伸的加载对MC3T3-E1成骨细胞中JNK和p38活性的影响,并观察到JNK和p38被机械应力激活。它们的激活方式取决于机械应力的大小和持续时间。在这项研究中,我们进行了DNA芯片和定量RT-PCR分析,以调查JNK和p38激活诱导的生物学输出。我们观察到,JNK和p38的机械应力增强激活诱导了许多基因的表达。这些基因之一是骨保护素,它是与骨代谢有关的主要基因。这些基因的清单还包括Fn14单核细胞(一种细胞因子受体家族成员,其配体已知由单核细胞和巨噬细胞产生),以及单核细胞趋化蛋白3。这些数据表明,机械应力激活的JNK和p38诱导了成骨细胞与骨髓衍生的单核细胞和巨噬细胞之间的细胞因子串扰,这可能在骨骼重塑中起关键作用。

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