Journal of Biomaterials Science, Polymer Edition ¶ 2002-01-01

Physicochemical properties and in vitro biocompatibility of PEO/PTMO multiblock copolymer/segmented polyurethane blends.

Jae Hyung Park, You Han Bae

Index: J. Biomater. Sci. Polym. Ed. 13(5) , 527-42, (2002)

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Abstract

A multiblock copolymer composed of poly(ethylene oxide) (PEO) and poly(tetramethylene oxide) (PTMO) and which forms a physical hydrogel was blended with Pellethane, a commercial segmented polyurethane (SPU) developed for various biomedical devices, to provide a PEO-rich surface with improved stability. The effect of the copolymer blending was evaluated with respect to surface hydrophilicity, long-term stability, mechanical properties, in vitro protein adsorption, and platelet adhesion. A small amount of the copolymer additive (5 wt%) significantly improved surface hydrophilicity, which was then gradually enhanced by increasing the amount of the copolymer in the blends. The blend films exhibited minimal extraction of the copolymer additive when exposed to a buffer solution for 2 months at 37 degrees C, resulting in less than 1 wt% weight loss of the films even with 30 wt% content of the copolymer in the blends. Although a certain degree of alteration in the mechanical properties was observed by increasing the copolymer content, the mechanical properties were well maintained for up to 10 wt% addition of the copolymer, when compared with the bare SPU. Protein adsorption was significantly reduced with a small amount of copolymer additive as low as 5 wt%. Fibrinogen, an adhesive protein for further cellular adhesion and activation, was effectively repelled by increasing the amount of copolymer additive. The platelet adhesion test revealed that the blend film surface reduced platelet adhesion and the degree of inhibition was proportional to the content of the additive, up to 30 wt%. The high molecular weight (Mw = 66,000) and compatible chemical structure of the copolymer with SPU made the surfaces PEO-rich and stable in an aqueous environment, resulting in an enhancement of the resistance to protein adsorption and platelet adhesion without a significant deterioration in physical properties.


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