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2003 Volume No 5 -
pages 61-67
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Title: Platelet adhesion studies on dipyridamole coated
polyurethane surfaces
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Authors: Y.B.J. Aldenhoff and L.H. Koole
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Address: Centre for Biomaterials Research, University
of Maastricht, PO Box 616, 6200 MD Maastricht, The Netherlands.
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E-mail: l.koole@bioch.unimaas.nl
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Key Words: Platelets, polyurethane, dipyridamole,
bloodcompatibility
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Publication date: 30th June 2003
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Abstract: Surface modification of polyurethanes
(PUs) by covalent attachment of dipyridamole (Persantin®)
is known to reduce adherence of blood platelets upon exposure
to human platelet rich plasma (PRP). This effect was investigated
in further detail. First platelet adhesion under static conditions
was studied with four different biomaterial surfaces: untreated
PU, PU immobilised with conjugate molecule 1, PU immobilised
with conjugate molecule 2, and PU immobilised with conjugate
molecule 3. In PU immobilised with 1 dipyridamole is directly
linked to the surface, in PU immobilised with 2 there is a
short hydrophilic spacer chain in between the surface and
the dipyridamole, while conjugate molecule 3 is merely the
spacer chain. Scanning electron microscopy (SEM) was used
to characterise platelet adhesion from human PRP under static
conditions, and fluorescence imaging microscopy was used to
study platelet adhesion from whole blood under flow. SEM experiments
encompassed both density measurements and analysis of the
morphology of adherent platelets. In the static experiments
the surface immobilised with 2 showed the lowest platelet
adherence. No difference between the three modified surfaces
emerged from the flow experiments. The surfaces were also
incubated with washed blood platelets and labeled with Oregon-Green
Annexin V. No capture of Oregon-Green Annexin V was seen,
implying that the adhered platelets did not expose any phosphatidyl
serine at their exteriour surface.
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