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Method of immobilization of carboxymethyl-dextran affects resistance to tissue and cell colonization
Authors:McLean  Johnson  Chatelier  Beumer  Steele  Griesser
Affiliation:

a CSIRO Molecular Science, Clayton Laboratory, Private Bag 10, Clayton South MDC, Clayton 3169, Australia

b CSIRO Molecular Science, Sydney Laboratory, PO Box 184, North Ryde 1670, Australia

c Cooperative Research Centre for Eye Research and Technology, University of New South Wales, Sydney 2052, Australia

Abstract:Coatings from carboxymethylated dextrans (CMDs) were fabricated, analyzed by XPS, and investigated for their ability to inhibit corneal epithelial tissue outgrowth and bovine corneal epithelial cell attachment and growth. CMDs with differing degrees of carboxymethyl substitution and various molecular weights were synthesized by the solution reaction of dextrans with bromoacetic acid under different reactant ratios. The CMD compounds thus obtained were attached onto aminated surfaces produced in two ways: by the plasma deposition of a coating from n-heptylamine vapour, and by the plasma deposition of an acetaldehyde coating onto whose surface aldehyde groups the polyamine compounds polylysine, polyethyleneimine and polyallylamine were immobilized to provide platforms for CMD immobilization. XPS spectra showed that the latter route produced thicker coatings than the former approach. CMD molecules attached directly onto the plasma-fabricated amine surface supported some tissue migration; the extent of carboxymethyl substitution and the molecular weight of the CMDs had little influence. For CMDs immobilized via polyamine spacers, on the other hand, tissue outgrowth was completely inhibited, and again there were no discernible effects from the extent of carboxymethyl substitution and the molecular weight of the CMDs. In assays involving cell attachment and growth, analogous observations were found. Thus, the mode of immobilization of these polysaccharide coatings is the dominant factor in their anti-fouling performance, suggesting that optimization of the architecture of polysaccharide coatings may be an important factor for maximizing their cell-repellent abilities.
Keywords:Polysaccharide  Carboxymethyldextran  Surface modification  Plasma polymer  Cell attachment  Tissue outgrowth
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