Regular drug-eluting stents versus the dedicated coronary bifurcation sirolimus-eluting BiOSS LIM® stent: the randomised, multicentre, open-label, controlled POLBOS II trial — Robert Gil (2016) | RDL Network
Regular drug-eluting stents versus the dedicated coronary bifurcation sirolimus-eluting BiOSS LIM® stent: the randomised, multicentre, open-label, controlled POLBOS II trial
EuroIntervention 12(11): e1404-e1412
Article 2016 English
Authors
RG
Robert Gil
JB
Jacek Bil
MG
Maik J. Grundeken
Abstract
1 min read
Aims:The aim of the POLBOS II randomised trial was to compare any regular drug-eluting stents (rDES) with the dedicated bifurcation sirolimus-eluting stent BiOSS LIM for the treatment of coronary bifurcation lesions.The secondary aim was to study the effect of final kissing balloon inflation (FKBI) on clinical outcomes.Methods and results: Between December 2012 and December 2013, 202 patients with stable coronary artery disease or non-ST-segment elevation acute coronary syndrome were randomly assigned 1:1 to treatment of the coronary bifurcation lesions either with the BiOSS LIM stent (n=102) or with an rDES (n=100).Coronary re-angiography was performed at 12 months.The primary endpoint was the composite of cardiac death, myocardial infarction (MI), and target lesion revascularisation (TLR) at 12 months.The target vessel was located in the left main in one third of the cases (35.3% in BiOSS and 38% in rDES).Side branch treatment was required in 8.8% (rDES) and 7% (BiOSS).At 12 months, the cumulative MACE incidence was similar in both groups (11.8% [BiOSS] vs. 15% [rDES, p=0.08]), as was the TLR rate (9.8% vs. 9% [p=0.8]).The binary restenosis rates were significantly lower in the FKBI subgroup of the BiOSS group (5.9% vs. 11.8%,p<0.05).Conclusions: MACE rates as well as TLR rates were comparable between the BiOSS LIM and rDES.At 12 months, cumulative MACE incidence was similar in both groups (11.8% vs. 15%), as was the TLR rate (9.8% vs. 9%).Significantly lower rates of restenosis were observed in the FKBI subgroup of the BiOSS group.
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