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Kyung Jae Jeong, Ph.D., Claes H. Dohlman, M.D., Ph.D., and Daniel S. Kohane, M.D., Ph.D. Harvard-MIT Health Sciences and Technology, Department of Anesthesiology, Children’s Hospital Boston, Harvard Medical School Massachusetts Eye and Ear Infirmary, Harvard Medical School *The authors have no financial interest in the subject matter of this poster. Khan et al. (2008) Cell migration Cell proliferation with minimal immune response ECM Production Adhesion Good biointegration will also reduce the danger of bacterial/fungal infection. Lee et al. Nature (2007) Lee et al. Adv. Materials (2009) Dopamine (or DOPA) is a major component of mussel adhesive protein and has good adhesive properties. Polydopamine coating can form on virtually all surfaces. Polydopamine coating can further be used to immobilize biological molecules which contain either thiol or amine groups at a high density. Chemistry is very simple. PMMA PMMA-RGD MTS assay on corneal epithelial cells Dopa-PMMA Dopa-PMMA-RGD Fluorescence micrographs of epithelial cells. Nucleus (blue) and actin cytoskeleton (red) PMMA PMMA-RGD MTS assay on keratocytes Dopa-PMMA Dopa-PMMA-RGD 1400 Keratocytes Epithelial Cells * Concentration of IL-6 (pg/mL) 1200 1000 800 * * * * ** 600 * * ** 400 200 0 PMMA Calcium assay. on human aortic smooth muscle cells (HASMC). Red point corresponds to polydopamine coating. Higher fluorescence response corresponds to higher cell contraction. PMMA-RGD Dp Dp+RGD TCP LPS IL-6 concentration from the cells seeded on various surfaces after 24 hours. TNF- α was not detected from neither cell types. Polydopamine coating does not release dopamine monomer (mass spectrometry) Minimal contraction of the aortic smooth muscle cells (Calcium Flux Assay). Not significantly high level of proinflammatory cytokines released from the cells seeded on the polydopamine surface (ELISA, IL-6 and TNF-α). PMMA Dopa-PMMA PMMA-RGD Dopa-RGD-PMMA A small PMMA cylinder was pressed onto collagen gel over night to see if there is any adhesion at the interface. PMMA PMMA Cylinder Collagen Gel Dopa-PMMA Polydopamine coating enhanced the proliferation of corneal epithelial cells and keratocytes in vitro. Polydopamine coating is not proinflammatory and is not expected to cause vascular constriction as its monomer would do. SEM images show ECM secretion from all surfaces. Both polydopamine-coated surfaces exhibited firm adhesion to collagen gel. Polydopamine coating may enhance the biointegration of Boston KPro when applied to the stem of the device.
