Ongoing foreign body reaction to subcutaneous implanted (heparin) modified Dacron in rats

Dacron‐containing heart valve repair devices trigger chronic inflammation characterized by the presence of activated macrophages, foreign body giant cells, and capsule formation. Upon blood contact, proinflammatory proteins adsorb to the material and provide a substrate for monocyte binding and diff...

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Published inJournal of biomedical materials research. Part A Vol. 68A; no. 3; pp. 423 - 427
Main Authors van Bilsen, Paul H. J., Popa, Eliane R., Brouwer, Linda A., Vincent, Judith, Taylor, Catherine E., de Leij, Lou F. M. H., Hendriks, Marc, van Luyn, Marja J. A.
Format Journal Article
LanguageEnglish
Published Hoboken Wiley Subscription Services, Inc., A Wiley Company 01.03.2004
Subjects
Adsorption
Animals
Coated Materials, Biocompatible - adverse effects
Dacron
foreign body reaction
Foreign-Body Reaction - chemically induced
Foreign-Body Reaction - pathology
Heart Valve Prosthesis - adverse effects
Heparin
implantation
Implants, Experimental - adverse effects
inflammation
Inflammation - chemically induced
Inflammation - pathology
Neovascularization, Pathologic - chemically induced
Polyethylene Terephthalates - adverse effects
Proteins - metabolism
Rats
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Summary:Dacron‐containing heart valve repair devices trigger chronic inflammation characterized by the presence of activated macrophages, foreign body giant cells, and capsule formation. Upon blood contact, proinflammatory proteins adsorb to the material and provide a substrate for monocyte binding and differentiation. Various heparin‐coated polymers have been shown to reduce adsorption of proinflammatory proteins in vitro and in vivo. In this study, the effect of knitted, heparin‐coated Dacron on the foreign body reaction was tested subcutaneously in rats. We hypothesized that the anti‐inflammatory effect of heparin would reduce monocyte recruitment and differentiation and therefore limit the inflammatory reaction. An ongoing foreign body reaction, characterized by the presence of foreign body giant cells and high vascularization, was observed in uncoated as well as (heparin‐)coated Dacron at up to 180 days of implantation. Also, a thin capsule was formed around each material up to this time. In conclusion, although heparin coatings might have an effect on the acute inflammatory response, we were not able to show a difference between heparin‐coated and uncoated Dacron after 180 days' implantation in rats. Further research needs to be conducted to assess the difference in proinflammatory protein adsorption between the tested materials and the effect this has on the long‐term foreign body reaction. © 2004 Wiley Periodicals, Inc. J Biomed Mater Res 68A: 423–427, 2004
Bibliography:istex:8A6FCA5E4A09033BC34303A515CE3408699A5786
ArticleID:JBM20069
ark:/67375/WNG-F3T69DTX-X
ISSN:1549-3296
1552-4965
DOI:10.1002/jbm.a.20069