Literature DB >> 15127387

Poly(carbonate urethane) and poly(ether urethane) biodegradation: in vivo studies.

Elizabeth M Christenson1, Mahrokh Dadsetan, Michael Wiggins, James M Anderson, Anne Hiltner.   

Abstract

Several strategies have been used to increase the biostability of medical-grade polyurethanes while maintaining biocompatibility and mechanical properties. One approach is to chemically modify or replace the susceptible soft segment. Currently, poly(carbonate urethanes) (PCUs) are being evaluated as a replacement of poly(ether urethanes) (PEUs) in medical devices because of the increased oxidative stability of the polycarbonate soft segment. Preliminary in vivo and in vitro studies have reported improved biostability of PCUs over PEUs. Although several studies have reported evidence of in vitro degradation of these new polyurethanes, there has been no evidence of significant in vivo degradation that validates a degradation mechanism. In this study, the effect of soft segment chemistry on the phase morphology, mechanical properties, and in vivo response of commercial-grade PEU and PCU elastomers was examined. Results from dynamic mechanical testing and infrared spectroscopy suggested that the phase separation was better in PCU as compared with PEU. In addition, the higher modulus and reduced ultimate elongation of PCU was attributed to the reduced flexibility of the polycarbonate soft segment. Following material characterization, the in vivo biostability and biocompatibility of PEU and PCU were studied using a subcutaneous cage implant protocol. The results from the cage implant study and cell culture experiments indicated that monocytes adhere, differentiate, and fuse to form foreign body giant cells on both polyurethanes. It is now generally accepted that the reactive oxygen species released by these adherent macrophages and foreign body giant cells initiate PEU biodegradation. Attenuated total reflectance-Fourier transform infrared analysis of explanted samples provided evidence of chain scission and crosslinking in both polyurethanes. This indicated that the PCU was also susceptible to biodegradation by agents released from adherent cells. These results reinforce the need to evaluate and understand the biodegradation mechanisms of PCUs. Copyright 2004 Wiley Periodicals, Inc. J Biomed Mater Res 69A: 407-416, 2004

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Year:  2004        PMID: 15127387     DOI: 10.1002/jbm.a.30002

Source DB:  PubMed          Journal:  J Biomed Mater Res A        ISSN: 1549-3296            Impact factor:   4.396


  21 in total

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4.  Improved Oxidative Biostability of Porous Shape Memory Polymers by Substituting Triethanolamine for Glycerol.

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5.  In vivo biostability of polymeric spine implants: retrieval analyses from a United States investigational device exemption study.

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Authors:  L E Tellier; J R Krieger; A L Brimeyer; A C Coogan; A A Falis; T E Rinker; A Schudel; S N Thomas; C D Jarrett; N J Willett; E A Botchwey; J S Temenoff
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8.  Determination of the in vivo degradation mechanism of PEGDA hydrogels.

Authors:  M B Browning; S N Cereceres; P T Luong; E M Cosgriff-Hernandez
Journal:  J Biomed Mater Res A       Date:  2014-02-13       Impact factor: 4.396

9.  The Latest Lessons Learned from Retrieval Analyses of Ultra-High Molecular Weight Polyethylene, Metal-on-Metal, and Alternative Bearing Total Disc Replacements.

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10.  3D printing and characterization of a soft and biostable elastomer with high flexibility and strength for biomedical applications.

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Journal:  J Mech Behav Biomed Mater       Date:  2020-01-23
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