Inhibition of neointima formation by a novel drug-eluting stent system that allows for dose-adjustable, multiple, and on-site stent coating

Rainer Wessely, Jörg Hausleiter, Cornelia Michaelis, Birgit Jaschke, Michael Vogeser, Stefan Milz, Boris Behnisch, Thomas Schratzenstaller, Magdalena Renke-Gluszko, Michael Stöver, Erich Wintermantel, Adnan Kastrati, Albert Schömig

Publikation: Beitrag in FachzeitschriftArtikelBegutachtung

136 Zitate (Scopus)

Abstract

Objective - The risk of in-stent restenosis can be considerably reduced by stents eluting cytostatic compounds. We created a novel drug-eluting stent system that includes several new features in the rapidly evolving field of stent-based drug delivery. Methods and Results - The aim of the present study was the preclinical evaluation of a stent-coating system permitting individual, on-site coating of stents with a unique microporous surface allowing for individualizable, dose-adjustable, and multiple coatings with identical or various compounds, designated ISAR (individualizable drug-eluting stent system to abrogate restenosis). Stents were coated with 0.75% rapamycin solution, and high-performance liquid chromatography (HPLC)-based determination of drug release profile indicated drug release for >21 days. Rapamycin-eluting microporous (REMP) stents implanted in porcine coronary arteries were safe. To determine the efficacy of REMP stents, this novel drug-eluting stent platform was compared with the standard sirolimus-eluting stent. At 30 days, in-stent neointima formation in porcine coronary arteries was similar in both groups, yielding a significant decrease of neointimal area and injury-dependent neointimal thickness compared with bare-metal stents. Conclusion - The ISAR drug-eluting stent platform as a novel concept for stent coating allows for a safe, effective, on-site stent coating process, thus justifying further clinical evaluation to decrease in-stent restenosis in humans.

OriginalspracheEnglisch
Seiten (von - bis)748-753
Seitenumfang6
FachzeitschriftArteriosclerosis, Thrombosis, and Vascular Biology
Jahrgang25
Ausgabenummer4
DOIs
PublikationsstatusVeröffentlicht - Apr. 2005

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