Pivotal, randomized US study of the Symbiot (TM) covered stent system in patients with saphenous vein graft disease: Eight-month angiographic and clinical results from the Symbiot III trial Article

Industry Collaboration International Collaboration

cited authors

  • Turco, Mark A., Buchbinder, Maurice, Popma, Jeffrey J., Weissman, Neil J., Mann, Tift, Doucet, Serge, Johnson, Warren L., Jr., Greenberg, Joel D., Leadley, Katrin, Russell, Mary E.

abstract

  • Objectives: The purpose of this study was to evaluate the clinical and angiographic outcomes of the Symbiot ePTFE covered stent versus bare metal stents (BMS) for the treatment of saphenous vein graft (SVG) disease. Background: The Symbiot stent was developed to reduce periprocedural complications, by potentially preventing distal embolization, and to serve as a possible barrier to cell migration, thus reducing restenosis. Methods: Symbiot III is a prospective, randomized trial of 400 patients at 45 US sites, with 201 patients in the Symbiot group and 199 in the BMS group. Randomization was stratified based on the intended use of embolic protection devices and glycoprotein IIb/IIIa inhibitors. The primary endpoint was percent diameter stenosis (%DS) as measured by quantitative coronary angiography at 8 months. Secondary endpoints included MACE (cardiac death, MI, TVR). Results: The groups were well matched for all baseline clinical and lesion characteristics. At 8 months, %DS was comparable between groups (30.9% Symbiot, 31.9% BMS, P = 0.80). Although the rates of binary restenosis in the stented segment were similar (29.1% Symbiot, 21.9% BMS, P = 0.17), more patients in the Symbiot group had binary restenosis at the proximal edge (9.0% Symbiot, 1.8% BMS, P = 0.0211). There was no difference in the incidence of MACE between groups (30.6% Symbiot, 26.6% BMS, P = 0.43). Conclusions: This study failed to show an advantage for the Symbiot stent in the treatment of degenerated SVGs. This PTFE covered stent does not appear to act as a barrier to prevent restenosis. (C) 2006 Wiley-Liss, Inc.

Publication Date

  • September 1, 2006

webpage

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start page

  • 379

end page

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volume

  • 68

issue

  • 3

WoS Citations

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