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    Hemocompatibility evaluation in vitro of methoxy polyethyleneglycol-polycaprolactone copolymer solutions

    Access Status
    Fulltext not available
    Authors
    Hu, Q.
    Zhang, Y.
    Wang, C.
    Xu, J.
    Wu, Ping
    Liu, Z.
    Xue, W.
    Date
    2016
    Type
    Journal Article
    
    Metadata
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    Citation
    Hu, Q. and Zhang, Y. and Wang, C. and Xu, J. and Wu, P. and Liu, Z. and Xue, W. 2016. Hemocompatibility evaluation in vitro of methoxy polyethyleneglycol-polycaprolactone copolymer solutions. Journal of Biomedical Materials Research - Part A. 104 (3): pp. 802-812.
    Source Title
    Journal of Biomedical Materials Research - Part A
    DOI
    10.1002/jbm.a.35594
    ISSN
    1549-3296
    School
    Department of Mechanical Engineering
    URI
    http://hdl.handle.net/20.500.11937/39698
    Collection
    • Curtin Research Publications
    Abstract

    Amphiphilic block copolymer methoxy polyethyleneglycol–polycaprolactone (mPEG–PCL) has attracted interest in the biomedical field, due to its water solubility and biodegradability. Nevertheless, the blood safety of mPEG–PCL copolymers has not been investigated in detail. Because mPEG–PCL copolymers introduced in vivo would inevitably interact with blood tissue, an investigation of possible interactions of mPEG–PCL with key blood components is crucial. We studied the effects of two mPEG–PCL copolymer solutions on blood coagulation, the morphology and lysis of human red blood cells (RBCs), the structure of plasma fibrinogen, complement activation, and platelet aggregation. We found that higher concentrations of the mPEG–PCL copolymers impaired blood clotting, and the copolymers had little impact on the morphology or lysis of RBCs. From the spectroscopy results, the copolymers affected the local microstructure of fibrinogen. The copolymers significantly activated the complement system in a concentration-dependent way. At higher concentrations, the copolymers impaired platelet aggregation, which may have been mediated by an inhibition of the arachidonic acid pathway. These findings provide important information that may be useful for the molecular design and biomedical applications of mPEG–PCL copolymers.

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