Publication | Closed Access
Mechanisms Involved in Osteoblast Response to Implant Surface Morphology
185
Citations
65
References
2001
Year
Tissue EngineeringEngineeringCell AdhesionBiomedical EngineeringCellular PhysiologyImplant Surface MorphologyBiomechanicsBone RemodelingCell Culture ModelMatrix BiologyCell SignalingMechanobiologySurface RoughnessCell BiologyDevelopmental BiologyCell-matrix InteractionSignal Transduction CascadesMedicineExtracellular Matrix
▪ Abstract Osteoblasts respond to surface topography with altered morphology, proliferation, and differentiation. The effects observed vary with cell culture model and the topographical features of the surface. In general, increased surface roughness is associated with decreased proliferation and increased differentiation. Cell responses to hormones, growth factors, and cytokines are altered as well, as is autocrine production of these factors. The cells interact with the surface via integrin receptors, and their expression is also surface roughness-dependent. Integrin binding to cell attachment proteins activates signal transduction cascades, including those mediated by protein kinase C and phospholipase A 2 . These signaling pathways are also used by regulatory factors, which results in synergistic responses. Prostaglandins are important mediators of the surface effects, and both constitutive and inducible cyclooxygenase are involved.
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