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Poly blood interfacing surface

Blood compatibility of PEG-modified surfaces was discussed in terms of the mobility of water molecules at the interface of hydrogel materices. The property and application of poly(N-isopropylacrylamide) and its copolymers as thermoresponsive hydrogel were also reviewed. [Pg.46]

Therefore, this chapter presents preliminary evidence indicating the effect and interrelationship between primary and secondary molecular motions on thrombogenesis, independent of morphological order and/or crystallinity. The polymer selected for this study was an amorphous elastomeric hydrophobic polymer of poly[(trifluoroethoxy) (fluoroalkoxy)phosphazene] (PNF) I (5, 6). The salient aspects of this polymer are that (1) the onset of the secondary molecular motions occurs between -160° and - 120°C (2) the side chain motion can be altered by irradiation (ultraviolet, electron beam, or gamma) (3) no apparent ultrastructure morphology exists (4) the side chains can be derivatized (5) and (5) the polymer can be readily coated onto our extracorporeal test shafts (7) and irradiated accordingly. Additionally, contact angle measurements of the homopolymer (8) and the PNF (9), 19.7 and 15.0 dyn/cm2, respectively, indicated that the fluorinated side chains comprised the surface to be interfaced in the extracorporeal blood studies. [Pg.180]


See other pages where Poly blood interfacing surface is mentioned: [Pg.46]    [Pg.47]    [Pg.16]    [Pg.219]    [Pg.46]    [Pg.304]    [Pg.205]    [Pg.316]    [Pg.96]    [Pg.137]    [Pg.207]    [Pg.234]    [Pg.244]    [Pg.246]    [Pg.255]    [Pg.269]    [Pg.325]    [Pg.233]    [Pg.561]    [Pg.566]    [Pg.486]    [Pg.1329]    [Pg.363]    [Pg.149]   
See also in sourсe #XX -- [ Pg.181 ]




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