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International journal of pharmaceutics ; 193(1): 123-127, December 1999. tab, gra
Artigo em Inglês | MedCarib | ID: med-17304

RESUMO

In order to achieve sustained antiplatelet effect from indomethacin, it was incorporated in a non-ionic surfactant vesicle (niosome). The objective was to study the effect of niosomal-encapsulated indomethacin on platelet function such as inhibition of aggrregation and ATP release induced by a variety of agonists (adenosine 5'-diphosphate (ADP)epinephrine, and arachidonic acid, ristocetine) and to explore the feasibilty of carrier-mediated drug delivery to the platelets. Multilamellar vesicles (niosomes) were prepared from Tween-60 by the lipid hydration method. Freshly prepared human platelet rich plasma (PRP) was used for aggregation/inhibition studies, the extent of which was observed as a change in light transmission measured by the Chronolog Aggregometer. The percent inhibition induced by the agonist ADP ranged from 28.21 ñ 0.28 at the æmol. level to 92.6 ñ 1.20 at 12.7 æmol. of the encapsulated drug while the same concentrations of the drug inhibited aggregation only to the extent of 13.75 ñ 0.13 and 36.82 ñ 0.57 percent respectively. A 100 percent inhibition of aggregation induced by arachidonic acid was achieved by niosomal indomethacin while inhibition by the free drug was 41.9 percent at equimolar concentrations. ATP release study showed that 100 percent inhibition was achieved by 8 æmol. of the encapsulated drug while inhibition by the free drug was 40.00 ñ 1.82 percent. Therefore, at equimolar doses, the niosomal drug proved to be more efficient in inhibiting platelet aggregation than the free drug, probably due to greater quantity of the drug reaching the specific site of inhibition in the interior of the platelets and acting directly on the cyclo-oxygenase system to prevent thromboxane formation(AU)


Assuntos
Indometacina , Agregação Plaquetária
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