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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00933270
Other study ID # SFA-1 US/EU
Secondary ID
Status Completed
Phase Phase 3
First received July 2, 2009
Last updated May 7, 2015
Start date July 2009
Est. completion date July 2014

Study information

Verified date May 2015
Source IDev Technologies, Inc.
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

This is a prospective, multicenter, non-randomized, single arm, pivotal trial.

The main objective of this study is to demonstrate the safety and effectiveness of the IDev SUPERA® Nitinol Stent System in treating subjects with obstructive superficial femoral artery (SFA) disease. The primary endpoint will be the primary patency of the SFA evaluated at 12 months. The outcome will be compared to a performance goal based on clinical trials of percutaneous transvenous angioplasty (PTA) alone.


Recruitment information / eligibility

Status Completed
Enrollment 325
Est. completion date July 2014
Est. primary completion date May 2014
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion Criteria:

1. Age greater than or equal to 18 years and of age of legal consent.

2. Women of child bearing potential must have a negative pregnancy test within 7 days prior to the index procedure.

3. Subject has lifestyle limiting claudication or rest pain (Rutherford-Becker scale 2-4) with a resting ankle-brachial index (ABI) less than or equal to 0.9. TBI (toe-brachial index) is performed only unable to assess ABI. TBI must be less than or equal to 0.7.

4. A single superficial femoral artery lesion with greater than 60% stenosis or total occlusion.

5. Stenotic lesion(s) or occluded length within the same vessel (one long or multiple serial lesions) greater than or equal to 40 mm to less than or equal to 140 mm. Reference vessel diameter (RVD) greater than or equal to 4.0 mm and less than or equal to 6.0 mm by visual assessment.

6. All lesions are to be located with the distal point at least 3 cm above the knee joint, defined as the distal end of the femur at the knee joint, and proximal point at least 2 cm below the origin of the profunda artery.

7. Patent infrapopliteal and popliteal artery, i.e., single vessel runoff or better with at least one of three vessels patent (less than 50% stenosis) to the ankle or foot.

8. The target lesion(s) can be successfully crossed with a guide wire and dilated.

9. Poor aortoiliac or common femoral "inflow" (i.e., angiographically defined greater than 50% stenosis of the iliac or common femoral artery) that would be deemed inadequate to support a femoropopliteal bypass graft must be successfully treated prior to treatment of the target lesion. This can be done just prior to treatment of the target lesion. Successful treatment is defined as less than 30% stenosis after either PTA or stenting of the inflow lesion. After treatment of the inflow lesion, the pressure gradient across the target lesion will be obtained and if the pressure gradient is greater than or equal to 20 mmHg, then the subject will be included in the study.

10. A subject with bilateral obstructive SFA disease is eligible for enrollment into the study. If a subject with bilateral disease is enrolled, the target limb will be selected at the Investigator's discretion, who may use the criteria of lesion length, percent stenosis, and/or calcification content. The contra-lateral procedure should not be done until at least 30 days after the index procedure (staged); however, if contralateral treatment is performed prior to treatment of the target lesion, the waiting period will be at least 14 days prior to the index procedure.

11. The subject is eligible for standard surgical repair, if necessary.

12. A subject who requires a coronary intervention should have it performed at least 7 days prior to the treatment of the target lesion.

13. Subject must provide written informed consent.

14. Subject must be willing to comply with the specified follow-up evaluation schedule.

Exclusion Criteria:

1. Thrombophlebitis or deep venous thrombus, within the previous 30 days.

2. Receiving dialysis or immunosuppressant therapy within the previous 30 days.

3. Thrombolysis of the target vessel within 72 hours prior to the index procedure, where complete resolution of the thrombus was not achieved.

4. Stroke within the previous 90 days.

5. Ipsilateral femoral aneurysm or aneurysm in the SFA or popliteal artery.

6. Required stent placement via a popliteal approach.

7. Required stent placement across or within 0.5 cm of the SFA/PFA bifurcation.

8. Procedures which are pre-determined to require stent-in-stent placement to obtain patency, such as in-stent restenosis.

9. Significant vessel tortuosity or other parameters prohibiting access to the lesion or 90° tortuosity which would prevent delivery of the stent device.

10. Required stent placement within 1 cm of a previously deployed stent.

11. Subject required a coronary intervention, and the coronary intervention was done less than 7 days prior to or planned within 30 days after the treatment of the target lesion.

12. Known allergies to any of the following: aspirin and all three of the following: clopidogrel bisulfate (Plavix®), ticlopidine (Ticlid®), and prasugrel (Effient®); heparin, nitinol (nickel titanium), or contrast agent, that cannot be medically managed.

13. Presence of thrombus prior to crossing the lesion.

14. Known or suspected active infection at the time of the procedure.

15. Presence of an ipsilateral arterial artificial graft.

16. Use of cryoplasty, laser, or atherectomy devices at the time of index procedure.

17. Restenotic lesion that had previously been treated by atherectomy, laser or cryoplasty within 3 months of the index procedure.

18. Subject has tissue loss, defined as Rutherford-Becker classification category 5 or 6.

19. History of neutropenia, coagulopathy, or thrombocytopenia that was unexplained or is considered to be at risk for reoccurrence.

20. Known bleeding or hypercoagulability disorder or significant anemia (Hb < 8.0) that cannot be corrected.

21. Subject has the following laboratory values:

1. platelet count less than 80,000/µL,

2. international normalized ratio (INR) greater than 1.5,

3. serum creatinine level greater than 2.0 mg/dL.

22. Subject requires general anesthesia for the procedure.

23. Subject is pregnant or plans to become pregnant during the study.

24. Subject has a co-morbid illness that may result in a life expectancy of less than 1 year.

25. Subject is participating in an investigational study of a new drug, biologic or device at the time of study screening. NOTE: Subjects who are participating in the long term follow-up phase of a previously investigational and now FDA-approved product are not excluded by this criterion.

Study Design

Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment


Intervention

Device:
SUPERA® Nitinol Stent System
Percutaneous Angioplasty of the Superior Femoral Artery with placement of a SUPERA® Stent at time of PTA

Locations

Country Name City State
United States Alice Heart Center Alice Texas
United States Austin Heart, P.A Austin Texas
United States Cardiovascular Specialist of Texas & North Austin Medical Center Austin Texas
United States Heritage Valley Health System Beaver Pennsylvania
United States North Cascade Cardiology, PLLC Bellingham Washington
United States ACT / CVRI & Cedar Sinai Medical Center Beverly Hills California
United States Willis Knighton Bossier Medical Center Bossier City Louisiana
United States Brigham and Women's Hospital Boston Massachusetts
United States Massachussetts General Hospital Boston Massachusetts
United States Bradenton Cardiology Center Bradenton Florida
United States Caritas-St. Elizabeth Medical Center Brighton Massachusetts
United States Deborah Heart Browns Mills New Jersey
United States Cardiology Consultants or Mainline Health System Bryn Mawr Pennsylvania
United States The Lindner Center for Research and Education at The Christ Hospital Cincinnati Ohio
United States University Hospital Cleveland Ohio
United States Ohio Health Research Institute / Riverside Methodist Hospital Columbus Ohio
United States Cardiovascular Research Institute of Dallas Dallas Texas
United States Cardiology Associates of Mobile, Inc. Fairhope Alabama
United States Clarian North / Heart Partners Fishers Indiana
United States Hunterdon Medical Center Flemington New Jersey
United States Plaza Medical Center of Fort Worth Fort Worth Texas
United States Greenville Hospital Systems Greenville South Carolina
United States Hartford Hospital Hartford Connecticut
United States Hattiesburg Clinic, P.A. Hattiesburg Mississippi
United States Terrebonne General Hospital Houma Louisiana
United States Hutchinson Hospital Corporation dba Promise Regional Medical Center Hutchinson Kansas
United States First Coast Cardiovascular Institute Jacksonville Florida
United States Wellmont Holston Valley Medical Center Kingsport Tennessee
United States Cardiovascular Institute of the South Lafayette Louisiana
United States Arkansas Heart Hospital Little Rock Arkansas
United States SJH Cardiology Associates Liverpool New York
United States Mount Sinai Medical Cente Miami Beach Florida
United States Columbia - St. Mary's Milwaukee Wisconsin
United States Cardiovascular Research of Northwest Indiana, LLC Munster Indiana
United States Vanderbilt Medical Center Nashville Tennessee
United States Robert Wood Johnson UMDNJ-RWJMS New Brunswick New Jersey
United States Yale University New Haven Connecticut
United States Lenox Hill Hospital New York New York
United States NYU Medical Center New York New York
United States Montgomery General Hospital Olney Maryland
United States Opelousas General Health System Opelousas Louisiana
United States Banner Good Samaritan Medical Center Phoenix Arizona
United States Maine Medical Center Portland Maine
United States The Miriam Hospital Providence Rhode Island
United States Louisiana Heart Center Slidell Louisiana
United States Tucson Medical Center Tucson Arizona
United States Forsyth Medical Center - Cardiovascular Research Winston-Salem South Carolina
United States Moffitt Heart & Vascular Group Wormleysburg Pennsylvania
United States Metro Health Hospital Wyoming Michigan

Sponsors (2)

Lead Sponsor Collaborator
IDev Technologies, Inc. Harvard Clinical Research Institute

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Primary Safety Endpoint: Freedom From Death, Target Lesion Revascularization (TLR), or Any Amputation of the Index Limb to 30 (±7) Days. 30 days Yes
Primary Primary Efficacy Endpoint: SFA Patency at 12 Months (± 30 Days), Defined as Freedom From Restenosis (PSVR = 2.0) and TLR. 12 months Yes
Secondary Technical (Lesion) Success Technical (lesion) success, defined as the attainment of <50% residual stenosis by Quantitative Angiography (QA) by any percutaneous method as determined by the Angiographic core laboratory. intraoperative Yes
Secondary Procedural Success Defined as device success with < 50% residual stenosis immediately after stent placement, mean trans-stenotic pressure gradient less than 5 mmHg, and without the occurrence of death, amputation or repeat revascularization of the target lesion during the hospital stay. intraoperative Yes
Secondary Device Success Device success, defined as achievement of a final residual diameter stenosis of <50% (by QA), using the assigned treatment only. intraoperative Yes
Secondary Secondary Safety Composite Endpoint Secondary safety endpoint was a combined rate of death at 30 (± 7) days, or TLR, index limb amputation, and an increase in Rutherford-Becker Classification by 2 classes at 12 months (± 30 Days) (comparing pre- to post-procedural assessments). 12 months (± 30 Days) Yes
Secondary Secondary Safety Endpoint Secondary safety endpoint was a combined rate of death at 30 (± 7) days, or TLR, index limb amputation, and an increase in Rutherford-Becker Classification by 2 classes (comparing pre- to post-procedural assessments). 24 months (± 30 Days) Yes
Secondary Stent Fracture Rate Stent fractures were analyzed by X-ray evaluation by a designated core laboratory and defined as type I, II, III, IV or V.
Stent fracture classification
Type I - a single strut fracture only.
Type II - multiple single nitinol stent fractures that can occur at different sites.
Type III - multiple nitinol stent fractures resulting in complete transverse linear fracture but without stent displacement.
Type IV - a complete transverse linear type III fracture with stent displacement.
Type V - a spiral dissection of a stent.
12 months (± 30 Days) Yes
Secondary Stent Fracture Rate Stent fractures were analyzed by X-ray evaluation by a designated core laboratory and defined as type I, II, III, IV or V. 24 months (± 30 Days) Yes
Secondary Ankle-brachial Index (ABI) Measurements on Target Limb A ratio of the highest ankle systolic blood pressure in one leg, usually measured with a 10 cm cuff at the ankle and using a continuous wave Doppler to detect return of blood flow in the anterior tibial and posterior tibial arteries, to the highest of either arm systolic blood pressure. Performed at rest with subject in supine position. Baseline No
Secondary Ankle-brachial Index (ABI) Measurements on Target Limb A ratio of the highest ankle systolic blood pressure in one leg, usually measured with a 10 cm cuff at the ankle and using a continuous wave Doppler to detect return of blood flow in the anterior tibial and posterior tibial arteries, to the highest of either arm systolic blood pressure. Performed at rest with subject in supine position. 1 month (± 7 Days) No
Secondary Ankle-brachial Index (ABI) on Target Limb A ratio of the highest ankle systolic blood pressure in one leg, usually measured with a 10 cm cuff at the ankle and using a continuous wave Doppler to detect return of blood flow in the anterior tibial and posterior tibial arteries, to the highest of either arm systolic blood pressure. Performed at rest with subject in supine position. 6 Months (± 14 Days) No
Secondary Ankle-brachial Index (ABI) on Target Limb A ratio of the highest ankle systolic blood pressure in one leg, usually measured with a 10 cm cuff at the ankle and using a continuous wave Doppler to detect return of blood flow in the anterior tibial and posterior tibial arteries, to the highest of either arm systolic blood pressure. Performed at rest with subject in supine position. 12 Months (± 30 Days) No
Secondary Target Lesion Revascularization (TLR) Defined as any repeat percutaneous intervention with or without evidence of stenosis = 50%, to improve blood flow inside or within 5 mm proximally and/or distally of the treated target lesion. 6 months (± 14 Days) Yes
Secondary Target Lesion Revascularization (TLR) Defined as any repeat percutaneous intervention with or without evidence of stenosis = 50%, to improve blood flow inside or within 5 mm proximally and/or distally of the treated target lesion. 12 months (± 30 Days) Yes
Secondary Target Lesion Revascularization (TLR) Defined as any repeat percutaneous intervention with or without evidence of stenosis = 50%, to improve blood flow inside or within 5 mm proximally and/or distally of the treated target lesion. 24 months (± 30 Days) Yes
Secondary SFA Patency: PSV Ratio < 2.0 Defined as freedom from restenosis [defined as diameter stenosis >50% with a peak systolic velocity (PSV) ratio = 2.0 as measured by duplex ultrasound] and TLR 6 Months (± 14 days) No
Secondary SFA Patency: PSV Ratio = 2.4 Defined as freedom from restenosis [defined as diameter stenosis >50% with a peak systolic velocity (PSV) ratio > 2.4 as measured by duplex ultrasound] and TLR 6 Months (± 14 days) No
Secondary SFA Patency: PSV Ratio = 2.4 Defined as freedom from restenosis [defined as diameter stenosis >50% with a peak systolic velocity (PSV) ratio > 2.4 as measured by duplex ultrasound] and TLR 12 Months (±30 days) No
Secondary Target Vessel Revascularization Defined as any repeat percutaneous intervention or bypass surgery performed in the target vessel at 6 months post-procedure. 6 months (± 14 days) Yes
Secondary Target Vessel Revascularization Defined as any repeat percutaneous intervention or bypass surgery performed in the target vessel at 12 months post-procedure. 12 months (±30 days) Yes
Secondary Target Vessel Revascularization Defined as any repeat percutaneous intervention or bypass surgery performed in the target vessel at 24 months post-procedure. 24 months (±30 days) Yes
Secondary Limb Ischemia Improvement: Rutherford Becker Scale Defined as an improvement in the Rutherford-Becker Clinical Improvement Scale of greater than or equal to one.
Grade +3 = Markedly improved. Symptoms are gone or markedly improved. ABI increased to >0.90.
Grade +2 = Moderately improved. Still symptomatic but with improvement in lesion category. ABI increased by 0.10 but not normalized.
Grade +1 = Minimally improved. Categorical improvement in symptoms without significant ABI increase (0.10 or less) or vice versa (but not both).
Grade 0 = No change. No categorical shift and less than 0.10 change in ABI. Grade -1 = Mildly worse. Either worsening of symptoms or decrease in ABI of 0.10.
Grade -2 = Moderate worsening. Deterioration of the subject's condition by one category or unexpected minor amputation.
Grade -3 = Marked worsening. Deterioration of the subject's condition by more than one category or major amputation.
1 month (± 7 days) No
Secondary Limb Ischemia Improvement: Rutherford Becker Scale Defined as an improvement in the Rutherford-Becker Clinical Improvement Scale of greater than or equal to one.
Grade +3 = Markedly improved. Symptoms are gone or markedly improved. ABI increased to >0.90.
Grade +2 = Moderately improved. Still symptomatic but with improvement in lesion category. ABI increased by 0.10 but not normalized.
Grade +1 = Minimally improved. Categorical improvement in symptoms without significant ABI increase (0.10 or less) or vice versa (but not both).
Grade 0 = No change. No categorical shift and less than 0.10 change in ABI. Grade -1 = Mildly worse. Either worsening of symptoms or decrease in ABI of 0.10.
Grade -2 = Moderate worsening. Deterioration of the subject's condition by one category or unexpected minor amputation.
Grade -3 = Marked worsening. Deterioration of the subject's condition by more than one category or major amputation.
12 Months (±30 days) No
Secondary Limb Ischemia Improvement: Rutherford Becker Scale Defined as an improvement in the Rutherford-Becker Clinical Improvement Scale of greater than or equal to one.
Grade +3 = Markedly improved. Symptoms are gone or markedly improved. ABI increased to >0.90.
Grade +2 = Moderately improved. Still symptomatic but with improvement in lesion category. ABI increased by 0.10 but not normalized.
Grade +1 = Minimally improved. Categorical improvement in symptoms without significant ABI increase (0.10 or less) or vice versa (but not both).
Grade 0 = No change. No categorical shift and less than 0.10 change in ABI. Grade -1 = Mildly worse. Either worsening of symptoms or decrease in ABI of 0.10.
Grade -2 = Moderate worsening. Deterioration of the subject's condition by one category or unexpected minor amputation.
Grade -3 = Marked worsening. Deterioration of the subject's condition by more than one category or major amputation.
24 Months (±30 days) No
Secondary Major Adverse Events (MAVE) Defined as a composite rate of
stent thrombosis,
clinically apparent distal embolization (defined as causing end-organ damage, e.g. lower extremity ulceration, tissue necrosis, or gangrene),
procedure-related arterial rupture,
acute limb ischemia,
target limb amputation,
procedure related bleeding event requiring transfusion.
30 days (±7 days) Yes
Secondary Major Adverse Events (MAVE) Defined as a composite rate of
stent thrombosis,
clinically apparent distal embolization (defined as causing end-organ damage, e.g. lower extremity ulceration, tissue necrosis, or gangrene),
procedure-related arterial rupture,
acute limb ischemia,
target limb amputation,
procedure related bleeding event requiring transfusion.
6 Months (±14 days) Yes
Secondary Major Adverse Events (MAVE) Defined as a composite rate of
stent thrombosis,
clinically apparent distal embolization (defined as causing end-organ damage, e.g. lower extremity ulceration, tissue necrosis, or gangrene),
procedure-related arterial rupture,
acute limb ischemia,
target limb amputation,
procedure related bleeding event requiring transfusion.
12 months (±30 days) Yes
Secondary Major Adverse Events (MAVE) Defined as a composite rate of
stent thrombosis,
clinically apparent distal embolization (defined as causing end-organ damage, e.g. lower extremity ulceration, tissue necrosis, or gangrene),
procedure-related arterial rupture,
acute limb ischemia,
target limb amputation,
procedure related bleeding event requiring transfusion.
24 months (±30 days) Yes
Secondary Index Limb Amputations Amputation was defined as the surgical removal of tissue anywhere from the toe to hip in the ipsilateral limb of the target site. 6 months (±14 days) Yes
Secondary Index Limb Amputations Amputation was defined as the surgical removal of tissue anywhere from the toe to hip in the ipsilateral limb of the target site. 12 months (±30 days) Yes
Secondary Index Limb Amputations Amputation was defined as the surgical removal of tissue anywhere from the toe to hip in the ipsilateral limb of the target site. 24 months (±30 days) Yes
Secondary Quality of Life Assessed (QoL) by SF-12 Questionnaire The Medical Outcomes Study 12-Item Short form survey (SF-12) was used to assess generic QoL. SF-12 Health Survey is validated measure using 12 questions to measure functional health and well-being from the patient's point of view. Scores on the scale are 0% (indicating poor perceived health status) to 100% (indicating excellent perceived health status) possible. Physical and mental summary scores from the SF-12 are scaled to a U.S. population mean of 50 and standard deviation of 10 (higher scores are better). Multiple groups have suggested minimum clinically important changes in SF-12 summary scores to be greater than 2-2.5 points, and moderate changes to be greater than 5 points. Baseline No
Secondary Quality of Life Assessed by SF-12 Questionnaire The Medical Outcomes Study 12-Item Short form survey (SF-12) was used to assess generic QoL.SF-12 Health Survey is validated measure using 12 questions to measure functional health and well-being from the patient's point of view. Scores on the scale are 0% (indicating poor perceived health status) to 100% (indicating excellent perceived health status) possible. Physical and mental summary scores from the SF-12 are scaled to a U.S. population mean of 50 and standard deviation of 10 (higher scores are better). Multiple groups have suggested minimum clinically important changes in SF-12 summary scores to be greater than 2-2.5 points, and moderate changes to be greater than 5 points. 6 Months (± 14 Days) No
Secondary Quality of Life Assessed by SF-12 Questionnaire The Medical Outcomes Study 12-Item Short form survey (SF-12) was used to assess generic QoL.SF-12 Health Survey is validated measure using 12 questions to measure functional health and well-being from the patient's point of view. Scores on the scale are 0% (indicating poor perceived health status) to 100% (indicating excellent perceived health status) possible. Physical and mental summary scores from the SF-12 are scaled to a U.S. population mean of 50 and standard deviation of 10 (higher scores are better). Multiple groups have suggested minimum clinically important changes in SF-12 summary scores to be greater than 2-2.5 points, and moderate changes to be greater than 5 points. 12 Months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Physical Limitation The PAQ assesses Peripheral arterial disease (PAD)-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Physical Limitation The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Physical Limitation The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Symptoms The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Symptoms The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Symptoms The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Symptom Stability The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Symptom Stability The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Symptom Stability The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Social Limitation The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Social Limitation The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Social Limitation The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Treatment Satisfaction The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Treatment Satisfaction The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Treatment Satisfaction The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Quality of Life The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Quality of Life The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Quality of Life The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Summary Score The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. Baseline No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Summary Score The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 6 months (± 14 Days) No
Secondary Quality of Life Assessed by Peripheral Artery Questionnaire (PAQ): Summary Score The PAQ assesses PAD-related physical limitation, symptoms, quality of life, social function and treatment satisfaction on 0-100 scales; higher scores are better. A threshold of 8 points has been proposed as a minimum clinically important difference for the PAQ summary scale. 12 months (± 30 Days) No
Secondary Clinical Category: Rutherford Becker Category and Clinical Description
0 = Asymptomatic, no hemodynamically significant occlusive disease, 1 = Mild claudication, 2 = Moderate claudication, 3 = Severe claudication, 4 = Ischemic rest pain, 5 = Minor tissue loss, non-healing ulcer, or focal gangrene with diffuse pedal ischemia, 6 = Major tissue loss, extending above transmetatarsal level, functional foot no longer salvageable
Baseline No
Secondary Clinical Category: Rutherford Becker Category and Clinical Description
0 = Asymptomatic, no hemodynamically significant occlusive disease, 1 = Mild claudication, 2 = Moderate claudication, 3 = Severe claudication, 4 = Ischemic rest pain, 5 = Minor tissue loss, non-healing ulcer, or focal gangrene with diffuse pedal ischemia, 6 = Major tissue loss, extending above transmetatarsal level, functional foot no longer salvageable
1 Month (± 7 Days) No
Secondary Clinical Category: Rutherford Becker Category and Clinical Description
0 = Asymptomatic, no hemodynamically significant occlusive disease, 1 = Mild claudication, 2 = Moderate claudication, 3 = Severe claudication, 4 = Ischemic rest pain, 5 = Minor tissue loss, non-healing ulcer, or focal gangrene with diffuse pedal ischemia, 6 = Major tissue loss, extending above transmetatarsal level, functional foot no longer salvageable
12 Months (± 30 Days) No
Secondary Clinical Category: Rutherford Becker Category and Clinical Description
0 = Asymptomatic, no hemodynamically significant occlusive disease, 1 = Mild claudication, 2 = Moderate claudication, 3 = Severe claudication, 4 = Ischemic rest pain, 5 = Minor tissue loss, non-healing ulcer, or focal gangrene with diffuse pedal ischemia, 6 = Major tissue loss, extending above transmetatarsal level, functional foot no longer salvageable
24 Months (± 30 Days) No
Secondary Clinical Improvement Compared With Baseline: Rutherford Becker Scale Clinical Improvement Compared With Baseline
Grade +3 = Markedly Improved, Grade +2 = Moderately Improved, Grade +1 = Minimally Improved, Grade 0 = No Change, Grade -1 = Mildly Worse, Grade -2 = Moderately Worsening, Grade -3 = Markedly Worsening
1 month (± 7 Days) No
Secondary Clinical Improvement Compared With Baseline: Rutherford Becker Scale Clinical Improvement Compared With Baseline
Grade +3 = Markedly Improved, Grade +2 = Moderately Improved, Grade +1 = Minimally Improved, Grade 0 = No Change, Grade -1 = Mildly Worse, Grade -2 = Moderately Worsening, Grade -3 = Markedly Worsening
12 Months (± 30 Days) No
Secondary Clinical Improvement Compared With Baseline: Rutherford Becker Scale Clinical Improvement Compared With Baseline
Grade +3 = Markedly Improved, Grade +2 = Moderately Improved, Grade +1 = Minimally Improved, Grade 0 = No Change, Grade -1 = Mildly Worse, Grade -2 = Moderately Worsening, Grade -3 = Markedly Worsening
24 Months (± 30 Days) No
Secondary Exercise Tolerance Test: Claudication Pain Distance Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. Baseline No
Secondary Exercise Tolerance Test: Claudication Pain Distance Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 1 month (± 7 Days) No
Secondary Exercise Tolerance Test: Claudication Pain Distance Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 12 months No
Secondary Exercise Tolerance Test: Claudication Pain Time (CPT) Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. Baseline No
Secondary Exercise Tolerance Test: Claudication Pain Time (CPT) Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 1 month (± 7 Days) No
Secondary Exercise Tolerance Test: Claudication Pain Time (CPT) Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 12 months (± 30 Days) No
Secondary Exercise Tolerance Test: Maximal Walking Distance Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. Baseline No
Secondary Exercise Tolerance Test: Maximal Walking Distance Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 1 month (± 7 Days) No
Secondary Exercise Tolerance Test: Maximal Walking Distance Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 12 months (± 30 Days) No
Secondary Exercise Tolerance Test: Maximal Walking Time Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. Baseline No
Secondary Exercise Tolerance Test: Maximal Walking Time Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 1 month (± 7 Days) No
Secondary Exercise Tolerance Test: Maximal Walking Time Absolute Claudication Distance (ACD) for this study was determined by the point of termination or maximum distance walked on the treadmill due to claudication. 12 months (± 30 Days) No
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