Literature DB >> 15264659

Macrophage behavior on surface-modified polyurethanes.

Jacqueline A Jones1, Mahrokh Dadsetan, Terry O Collier, Michael Ebert, Ken S Stokes, Robert S Ward, P Anne Hiltner, James M Anderson.   

Abstract

Adherent macrophages and foreign body giant cells (FBGCs) are known to release degradative molecules that can be detrimental to the long-term biostability of polyurethanes. The modification of polyurethanes using surface modifying endgroups (SMEs) and/or the incorporation of silicone into the polyurethane soft segments may alter macrophage adhesion, fusion and apoptosis resulting in improved long-term biostability. An in vitro study of macrophage adhesion, fusion and apoptosis was performed on polyurethanes modified with fluorocarbon SMEs, polyethylene oxide (PEO) SMEs, or poly(dimethylsiloxane) (PDMS) co-soft segment and SMEs. The fluorocarbon SME and PEO SME modifications were shown to have no effect on macrophage adhesion and activity, while silicone modification had varied effects. Macrophages were capable of adapting to the surface and adhering in a similar manner to the silicone-modified and unmodified polyurethanes. In the absence of IL-4, macrophage fusion was comparable on the modified and unmodified polyurethanes, while macrophage apoptosis was promoted on the silicone modified surfaces. In contrast, when exposed to IL-4, a cytokine known to induce FBGC formation, silicone modification resulted in more macrophage fusion to form foreign body giant cells. In conclusion, fluorocarbon SME and PEO SME modification does not affect macrophage adhesion, fusion and apoptosis, while silicone modification is capable of mediating macrophage fusion and apoptosis. Silicone modification may be utilized to direct the fate of adherent macrophages towards FBGC formation or cell death through apoptosis.

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Year:  2004        PMID: 15264659     DOI: 10.1163/156856204323046843

Source DB:  PubMed          Journal:  J Biomater Sci Polym Ed        ISSN: 0920-5063            Impact factor:   3.517


  14 in total

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Review 3.  Mesh biocompatibility: effects of cellular inflammation and tissue remodelling.

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4.  Vitronectin is a critical protein adhesion substrate for IL-4-induced foreign body giant cell formation.

Authors:  Amy K McNally; Jacqueline A Jones; Sarah R Macewan; Erica Colton; James M Anderson
Journal:  J Biomed Mater Res A       Date:  2008-08       Impact factor: 4.396

Review 5.  Biocompatible materials for continuous glucose monitoring devices.

Authors:  Scott P Nichols; Ahyeon Koh; Wesley L Storm; Jae Ho Shin; Mark H Schoenfisch
Journal:  Chem Rev       Date:  2013-02-07       Impact factor: 60.622

Review 6.  Chronic inflammation in biomaterial-induced periprosthetic osteolysis: NF-κB as a therapeutic target.

Authors:  Tzu-hua Lin; Yasunobu Tamaki; Jukka Pajarinen; Heather A Waters; Deanna K Woo; Zhenyu Yao; Stuart B Goodman
Journal:  Acta Biomater       Date:  2013-10-01       Impact factor: 8.947

7.  Histological assessment of tissue from large human bone defects repaired with β-tricalcium phosphate.

Authors:  Tomas Kucera; Pavel Sponer; Karel Urban; Ales Kohout
Journal:  Eur J Orthop Surg Traumatol       Date:  2013-10-05

8.  In vitro evaluation of the PEtU-PDMS material immunocompatibility: the influence of surface topography and PDMS content.

Authors:  D Spiller; C Mirtelli; P Losi; E Briganti; S Sbrana; S Counoupas; S Kull; S Tonlorenzi; G Soldani
Journal:  J Mater Sci Mater Med       Date:  2009-12       Impact factor: 3.896

9.  The foreign body reaction in T-cell-deficient mice.

Authors:  Analiz Rodriguez; Sarah R Macewan; Howard Meyerson; James T Kirk; James M Anderson
Journal:  J Biomed Mater Res A       Date:  2009-07       Impact factor: 4.396

10.  Instability of self-assembled monolayers as a model material system for macrophage/FBGC cellular behavior.

Authors:  Jacqueline A Jones; L Abby Qin; Howard Meyerson; Il Keun Kwon; Takehisa Matsuda; James M Anderson
Journal:  J Biomed Mater Res A       Date:  2008-07       Impact factor: 4.396

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