Literature DB >> 19615736

Fibronectin-mediated endothelialisation of chitosan porous matrices.

Isabel F Amaral1, Ronald E Unger, Sabine Fuchs, Ana M Mendonça, Susana R Sousa, Mário A Barbosa, Ana P Pêgo, C J Kirkpatrick.   

Abstract

Chitosan (Ch) porous matrices were investigated regarding their ability to be colonized by human microvascular endothelial cells (HPMEC-ST1.6R cell line) and macrovascular endothelial cells namely HUVECs. Specifically we assessed if previous incubation of Ch in a fibronectin (FN) solution was effective in promoting endothelial cell (EC) adhesion to Ch matrices with different degrees of acetylation (DAs). Upon FN physiadsorption, marked differences were found between the two DAs investigated, namely DA 4% and 15%. While cell adhesion was impaired on Ch with DA 15%, ECs were able to not only adhere to Ch with DA 4%, but also to spread and colonize the scaffolds, with retention of the EC phenotype and angiogenic potential. To explain the observed differences between the two DAs, protein adsorption studies using (125)I-FN and immunofluorescent labelling of FN cell-binding domains were carried out. In agreement with the higher cell numbers found, scaffolds with DA 4% revealed a higher number of exposed FN cell-binding domains as well as greater ability to adsorb FN and to retain and exchange adsorbed FN in the presence of competitive proteins. These findings suggest that the DA is a key parameter modulating EC adhesion to FN-coated Ch by influencing the adsorbed protein layer.

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Year:  2009        PMID: 19615736     DOI: 10.1016/j.biomaterials.2009.06.056

Source DB:  PubMed          Journal:  Biomaterials        ISSN: 0142-9612            Impact factor:   12.479


  11 in total

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8.  In vivo biocompatibility study of electrospun chitosan microfiber for tissue engineering.

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10.  Kinetics and isotherm of fibronectin adsorption to three-dimensional porous chitosan scaffolds explored by ¹²⁵I-radiolabelling.

Authors:  Isabel F Amaral; Susana R Sousa; Ismael Neiva; Lara Marcos-Silva; Charles J Kirkpatrick; Mário A Barbosa; Ana P Pêgo
Journal:  Biomatter       Date:  2013-04-29
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