Blood Compatibility of Poly(2-methoxyethyl acrylate)-Design of Novel Biointerfaces

DOI 1 Citations Open Access
  • TANAKA Masaru
    Molecular Device Laboratory, Research Institute for Electronic Science (RISE), Hokkaido University, and PRESTO, Japan Science and Technology Corporation (JST)

Bibliographic Information

Other Title
  • 新しい血液適合性高分子の設計とバイオメディカルインターフェイスの構築

Description

The Poly (2-methoxyethyl acrylate) (PMEA) surface shows excellent blood compatibility with respect to the coagulation, complement, and platelet systems when compared with other polymer surfaces. To clarify the reasons for this good compatibility, kinetics of protein adsorption and desorption on PMEA surface, and the structure of water in the hydrated PMEA were investigated. Poly (2-hydroxyethyl methacrylate) (PHEMA) and polyacrylate analogs were used as references. The amount of protein adsorbed onto PMEA was very small, and close to that adsorbed onto PHEMA. PMEA showed the low denaturation and the high dissociation rate constant of the proteins adsorbed onto PMEA. The hydrated water in PMEA could be classified into three types; free water, freezing-bound water, and non-freezing water. Cold crystallization of water in the heating process was clearly observed at-42°C. This cold crystallization is interpreted as the phase transition from the amorphous ice to the crystal ice that belongs to the freezing-bound water in PMEA. We hypothesized that the freezingbound water layer between free water and non-freezing water was an important factor for the excellent blood compatibility of PMEA. The present study also describes the fabrication and characterization of highly regular porous polymer films formed by a simple casting technique. The porous film with controlled pore size from 0.2 to 100μm is used for tissue engineering scaffolds and biomedical devices.

Journal

  • KOBUNSHI RONBUNSHU

    KOBUNSHI RONBUNSHU 60 (8), 415-427, 2003

    The Society of Polymer Science, Japan

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Details 詳細情報について

  • CRID
    1390001206522393728
  • NII Article ID
    130003837841
  • DOI
    10.1295/koron.60.415
  • ISSN
    18815685
    03862186
  • Text Lang
    ja
  • Data Source
    • JaLC
    • Crossref
    • CiNii Articles
    • OpenAIRE
  • Abstract License Flag
    Disallowed

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