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Randomized Controlled Trial
. 2015 Jan 6;131(1):74-81.
doi: 10.1161/CIRCULATIONAHA.114.013520. Epub 2014 Nov 19.

Long-term efficacy and safety of biodegradable-polymer biolimus-eluting stents: main results of the Basel Stent Kosten-Effektivitäts Trial-PROspective Validation Examination II (BASKET-PROVE II), a randomized, controlled noninferiority 2-year outcome trial

Christoph Kaiser  1 Soeren Galatius  2 Raban Jeger  2 Nicole Gilgen  2 Jan Skov Jensen  2 Christoph Naber  2 Hannes Alber  2 Maria Wanitschek  2 Franz Eberli  2 David J Kurz  2 Giovanni Pedrazzini  2 Tiziano Moccetti  2 Hans Rickli  2 Daniel Weilenmann  2 André Vuillomenet  2 Martin Steiner  2 Stefanie Von Felten  2 Deborah R Vogt  2 Kim Wadt Hansen  2 Peter Rickenbacher  2 David Conen  2 Christian Müller  2 Peter Buser  2 Andreas Hoffmann  2 Matthias Pfisterer  2 BASKET-PROVE II study group
Collaborators, Affiliations
Randomized Controlled Trial

Long-term efficacy and safety of biodegradable-polymer biolimus-eluting stents: main results of the Basel Stent Kosten-Effektivitäts Trial-PROspective Validation Examination II (BASKET-PROVE II), a randomized, controlled noninferiority 2-year outcome trial

Christoph Kaiser et al. Circulation. .

Abstract

Background: Biodegradable-polymer drug-eluting stents (BP-DES) were developed to be as effective as second-generation durable-polymer drug-eluting stents (DP-DES) and as safe >1 year as bare-metal stents (BMS). Thus, very late stent thrombosis (VLST) attributable to durable polymers should no longer appear.

Methods and results: To address these early and late aspects, 2291 patients presenting with acute or stable coronary disease needing stents ≥3.0 mm in diameter between April 2010 and May 2012 were randomly assigned to biolimus-A9-eluting BP-DES, second-generation everolimus-eluting DP-DES, or thin-strut silicon-carbide-coated BMS in 8 European centers. All patients were treated with aspirin and risk-adjusted doses of prasugrel. The primary end point was combined cardiac death, myocardial infarction, and clinically indicated target-vessel revascularization within 2 years. The combined secondary safety end point was a composite of VLST, myocardial infarction, and cardiac death. The cumulative incidence of the primary end point was 7.6% with BP-DES, 6.8% with DP-DES, and 12.7% with BMS. By intention-to-treat BP-DES were noninferior (predefined margin, 3.80%) compared with DP-DES (absolute risk difference, 0.78%; -1.93% to 3.50%; P for noninferiority 0.042; per protocol P=0.09) and superior to BMS (absolute risk difference, -5.16; -8.32 to -2.01; P=0.0011). The 3 stent groups did not differ in the combined safety end point, with no decrease in events >1 year, particularly VLST with BP-DES.

Conclusions: In large vessel stenting, BP-DES appeared barely noninferior compared with DP-DES and more effective than thin-strut BMS, but without evidence for better safety nor lower VLST rates >1 year. Findings challenge the concept that durable polymers are key in VLST formation.

Clinical trial registration url: http://www.clinicaltrials.gov. Unique identifier: NCT01166685.

Keywords: antiplatelet drugs; clinical trial; coronary artery disease; coronary thrombosis; drug-coated stents; drug-eluting stents.

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