A Safety and Efficacy Study of the Dynalink®-E Everolimus Eluting Peripheral Stent System

Abbott Medical Devices104 enrolled

Overview

The purpose of this first-in-man study is to evaluate the safety and performance of the Dynalink®-E everolimus eluting peripheral stent system for the treatment of patients with atherosclerotic de novo or restenotic native superficial femoral and proximal popliteal lesions. Abbott Vascular is ceasing data analysis of the STRIDES Clinical Trial after 2 years. The decision to discontinue the study is not related to any safety concern. The rationale for this proposal is based on the following considerations: The performance of DYNALINK-E from STRIDES shows no device- or procedure-related deaths and no stent fractures, and the rate of additional revascularizations has been stable since approximately 14 months after the procedure. Evaluations of the bare metal nitinol DYNALINK and ABSOLUTE stents in the clinical literature show low rates of death, reintervention and stent fracture, which are consistent with STRIDES and demonstrate the safety of the nitinol stent platform of the DYNALINK-E. Long-term animal studies show no concerns with the drug or polymer coating of DYNALINK-E - everolimus tissue concentration drops below the quantifiable limit by approximately 17 months after implant, and vascular response to the coating is normal with widely patent lumens and struts incorporated into vessel tissue. The safety and performance of the DYNALINK-E has been substantiated by its clinical and pre-clinical data, and by the clinical data of similar products. Given the demonstrated mechanical integrity of the stent along with the evidence of a healthy long-term vascular response, there is a reasonable expectation of continued low event rates.

A prospective, Non-Randomized, Single-arm, Multi-center, Clinical Study to Evaluate the Safety and Performance of the Dynalink®-E, Everolimus Eluting Peripheral Stent System for the Treatment of Atherosclerotic de Novo or Restenotic Native Superficial Femoral and Proximal Popliteal Artery Lesions.

Study Type

INTERVENTIONAL

Allocation

NON_RANDOMIZED

Purpose

TREATMENT

Masking

NONE

Eligibility

Sex: ALLMin age: 18 Years

Medical Language ↔ Plain English

Inclusion Criteria: * Rutherford Becker Category 2-5 * Single de novo or restenotic lesion in the superficial femoral or proximal popliteal artery * Disease segment length 30-170 mm * \>50% diameter stenosis or total occlusion * Target reference vessel diameter 4.3-7.3 mm Exclusion Criteria: * Target lesion previously treated with stent or surgery * Rutherford Becker Category 0, 1, or 6 * Immunosuppressive disorder or currently receiving immunosuppressive agents * Serum creatinine \>2.5 mg/dl

Locations (10)

Landeskrankenhaus Klagenfurt

Klagenfurt, Austria

Allgemeines Krankenhaus der Stadt Wien- AKH Wien

Vienna, Austria

Sint Blasius Hospital

Dendermonde, Belgium

ZOL St. Jan

Ghent, Belgium

University Hospital

Ghent, Belgium

Herzzentrum Bad Krozingen

Bad Krozingen, Germany

The Jewish Hospital Berlin

Berlin, Germany

Herzzentrum Leipzig

Leipzig, Germany

University Hospital Tübingen

Tübingen, Germany

Casa di Cura di Montevergine

Mercogliano, Italy

Outcomes

Primary Outcomes

In-stent binary restenosis (>50% stenosis), as measured by duplex ultrasound

Time frame: 6 months

Secondary Outcomes

Angiographic in-stent binary restenosis rate (>50%)

Time frame: 12 months

Angiographic mean in-stent late loss, in-stent mean minimum lumen diameter (MLD), percent diameter stenosis

Time frame: 12 months

Primary, and secondary patency

Time frame: 1, 6, 12, 18 months, 2, 3, 4, 5 years