Nur fatmawati
16611047
Examination of the in vivo mechanism of late drug-eluting stent thrombosis.
Although , stent thrombosis
remains a severe complication after stent implantation owing to its high
morbidity and mortality. Since the introduction of drug-eluting stents (DES),
most interventional centers have noted stent thrombosis up to 3 years after implantation,
a complication rarely seen with bare-metal stents. Some data from large
registries and meta-analyses of randomized trials indicate a higher risk for
DES thrombosis, whereas others suggest an absence of such a risk. Several
factors are associated with an increased risk of stent thrombosis, including
the procedure itself (stent malapposition and/or underexpansion, number of
implanted stents, stent length, persistent slow coronary blood flow, and
dissections), patient and lesion characteristics, stent design, and premature
cessation of antiplatelet drugs. Drugs released from DES exert distinct
biological effects, such as activation of signal transduction pathways and
inhibition of cell proliferation. As a result, although primarily aimed at preventing
vascular smooth muscle cell proliferation and migration (ie, key factors in the
development of restenosis), they also impair reendothelialization, which leads
to delayed arterial healing, and induce tissue factor expression, which results
in a prothrombogenic environment.
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