Compare the Effectiveness and Safety of Genoss® DCB and IN.PACT Admiral® DCB in Patients With Peripheral Artery Disease

Genoss

Status

Completed

Conditions

Peripheral Artery Disease

De Novo Stenosis

Treatments

Device: Genoss® DCB

Device: IN.PACT Admiral® DCB

Study type

Interventional

Funder types

Industry

Identifiers

NCT05134545

CSP-DS1411

Details and patient eligibility

About

The purpose of this clinical trial is to demonstrate the non-inferiority of GENOSS DCB versus IN.PACT Admiral DCB on late lumen loss 6 months after the procedure in patients with de novo or non-stented restenotic lesions of the superficial femoral artery and popliteal artery and to evaluate the safety.

This clinical trial will be conducted on a total of 118 patients at 11 domestic institutions (taking into account the dropout rate of 30%).

Full description

In this clinical trial, IN.PACT Admiral, which is the most similar to GENOSS DCB, a test device, and the product type and purpose of use, and whose effectiveness has already been proven through numerous clinical studies, was selected as a control product.

Due to the nature of this clinical trial, the investigator cannot be blinded to the treatment method to which the subject is assigned, so it is designed as a double-blind design in which only the subject and the independent evaluator are blinded.

For efficacy and safety evaluation, follow-up is performed up to 12 months after procedure of the clinical trial medical device.

The primary endpoint of the effectiveness evaluation was performed by an independent evaluator and CT angiography at 6 months of in-segment late lumen loss.

It is evaluated the revascularization rate, Rutherford classification, the amount of change in ABI or TBI at 1, 6, and 12 months, the procedural success rate during the clinical trial period, and the device success rate immediately after the procedure.

Safety evaluation is confirmed through all adverse events, MAE (Major adverse event), vital signs, physical examination and laboratory test results that occur to the subject during the clinical trial period after procedure of the clinical trial medical device.

Enrollment

119 patients

Sex

All

Ages

19 to 85 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

≥ 19 years and ≤ 85 years of age
Documented ischemia with Rutherford classification 2, 3, 4 or 5
Target lesion is in the SFA and/or PPA
Reference vessel diameter ≥ 4 mm and ≤ 7 mm by visual estimate
Angiographic evidence that target lesion consists of a single de novo or non-stented restenotic lesion;
- 70% - 99% occluded with total lesion length ≥ 40 mm and ≤ 300 mm
- 100% occluded with total lesion length ≤ 100 mm
- Combination lesions (a non-occlusive lesion that includes a totally occluded segment along its length) are eligible provided that (1) the combined lesion length is ≥ 40 mm and ≤ 300 mm and (2) the totally occluded segment is not greater than 100 mm in length.
- Tandem or adjacent lesions are treated as a single lesion, the gap between the lesions is ≤ 30 mm, and the total combined lesion length including the distance between the lesions is ≥ 40 mm and ≤ 300 mm

Exclusion criteria

Stroke or STEMI within 3 months prior to enrollment
Acute thrombosis or acute aneurysm in the target lesion
History of or planning to have a major amputation in the leg
Failure to successfully cross the target lesion with a guidewire
Poor distal run-off artery to the ankle or lower
Known allergies or sensitivities to paclitaxel, shellac, vitamin E, heparin, aspirin, other anticoagulant/antiplatelet therapies or contrast agent
Target lesion is one of the following;
- In-stent restenosis (ISR)
- Restenosis after DCB procedure
- Previously treated with bypass surgery
- Severe concentric calcified lesions on angiography where pre-dilation cannot be performed or failed, and the procedure for the device for clinical trials is inadequate
Those who need stenting due to vascular dissection that restricts blood flow of Grade D or higher after pre-dilation
Any major (e.g., cardiac, peripheral, abdominal) intervention (including in the contralateral SFA/PPA) planned within 30 days post index procedure
Life expectancy, in the Investigator's opinion, is less than 12 months
Chronic renal insufficiency with serum creatinine > 2.5 mg/dL