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The objective of this prospective, multi-center, single arm study is to obtain further data on the safety and performance of the StellarexTM 0.014" OTW Drug-coated Angioplasty Balloon in the treatment of lesions in "below the knee" popliteal (P3 segment) and infra-popliteal arteries according to the Instructions for Use in Rutherford-Becker Classification (RCC) 3, 4 and 5 patient populations. This study will be conducted in Europe across up to 10 centers in up to 75 subjects. Office visits will occur at 30 days, 6, 12, and 24 months post-index procedure.
There is a significant amount of evidence that the use of Paclitaxel-coated balloons in the treatment of peripheral arterial disease (PAD) has demonstrated favorable outcomes when used to treat lesions in the superficial femoral and popliteal arteries. For subjects with lesions in the infrapopliteal arteries, which includes lesions in the mid to distal popliteal artery and below, a smaller profile balloon is necessary. Typically, lesions in the SFA and proximal popliteal arteries are treated by larger diameter balloons and larger sized guidewires (most commonly 0.018" or 0.035") which are too large for vessels below-the-knee. For this reason, the Stellarex™ 0.014" OTW Drug-coated Angioplasty Balloon was developed as a line extension to the Stellarex™ 0.035" device in order to accommodate the treatment of these smaller vessels. The Stellarex™ 0.014" balloon has the same drug concentration and is manufactured using a similar method as the Stellarex™ 0.035" device. Additionally, the Stellarex™ 0.035" and 0.014" balloon share a common balloon diameter of 4 mm, a size which was used to treat lesions throughout the popliteal artery in the previous Stellarex 0.035" studies. For the reasons noted above, equivalence between the two devices has been demonstrated. Furthermore, it is believed that the 0.014" device will not demonstrate any performance differences nor change the anticipated or residual risks.
In conclusion, the current study has been developed in agreement with post-market requirements as per the Post Market Clinical Follow up (PMCF) plan. The prospective design of the study, the sample size and the selected outcomes will be able to provide the additional clinical information to support the safe use and performance of the Stellarex 0.014" device in the intended population of patients with below-the-knee arterial disease.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Treatment | Experimental | StellarexTM 0.014 OTW Drug-coated Angioplasty Balloon (Stellarex Balloon) |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| StellarexTM 0.014" Over-The-Wire Drug-coated Angioplasty Balloon | Combination Product | The Stellarex balloon (0.014") is indicated for the treatment of de-novo or re-stenotic lesions in the lower extremities to establish blood flow and to maintain vessel patency. |
| Measure | Description | Time Frame |
|---|---|---|
| Primary Safety Endpoint-Composite Major Adverse Limb Events (MALE) + perioperative death (POD); the composite is the number of participants who do not have MALE or POD at 30 days | Major Adverse Limb Event (MALE) is defined as the composite of either major amputation or major re-intervention through 30 days of the index procedure. Major re-intervention is defined as creation of a new surgical bypass graft, the use of thrombectomy or thrombolysis or a major surgical graft revision such as a jump graft or an interposition graft. This is a single endpoint as it is a composite only subjects who do not have MALE or POD will be counted toward this endpoint MALE is defined as the composite of either major amputation or major re-intervention through 30 days of the index procedure. Major re-intervention is defined as creation of a new surgical bypass graft, the use of thrombectomy or thrombolysis or a major surgical graft revision such as a jump graft or an interposition graft. POD is all-cause death through 30 days of the index procedure. | 30 days |
| Primary Performance Endpoint-Composite patency + limb salvage through 6 months; the composite is the number of participants with patency and limb salvage at 6 months | Patency defined as freedom from occluded target lesions (flow/no flow) verified by duplex ultrasound and clinically-driven target lesion revascularization (CD-TLR) Freedom from major amputation in the Target Limb This is a single endpoint as only subjects with both patency and limb salvage will be considered for this endpoint. | 6 months |
| Measure | Description | Time Frame |
|---|---|---|
| Major adverse event (MAE) rate at 6,12, and 24 months post index procedure | Defined as a composite rate of all-cause death, target limb major amputation and CD-TLR | 6 Months |
| Major adverse event (MAE) rate at 6,12, and 24 months post index procedure |
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Inclusion Criteria:
Exclusion Criteria:
Subjects with any medical condition that would make him/her inappropriate for treatment with the Stellarex balloon as per the Instructions for Use (IFU) or in the opinion of the investigator.
Has impaired renal function defined as serum creatinine >2.5 mg/dl that cannot be adequately pre-treated or subjects on dialysis.
Subjects already enrolled in other investigational (interventional) studies that would interfere with study endpoints.
Subjects that in the judgment of the investigator would require treatment of the contralateral limb within 3 days prior to the index procedure or 30 days after. Note: Unless contralateral treatment is required to facilitate adequate access to the target lesion (e.g. contralateral iliac).
Previous or planned surgical or catheter-based procedure within 3 days before or 30 days after the index procedure. Note: This excludes successful inflow artery treatment within the same hospitalization or a documented preplanned minor amputation.
Prior endovascular treatment of the target lesion within three (3) months of the index procedure.
Prior stent placement in the target lesion(s).
Single focal lesion < 4cm in length in the absence of additional treatable popliteal or infra-popliteal lesions.
Subjects confined to bed that are completely non-ambulatory.
For RCC 5 subjects: Non-arterial ulcers such as venous ulcers, neurotrophic ulcers, heel pressure ulcers, ulcers potentially involving calcaneus region or ulcers in the proximal one-half of the foot or higher (from mid-foot and higher going up the leg).
Subjects scheduled to undergo a planned major amputation.
Presence of concentric calcification that precludes adequate vessel preparation per IFU.
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| Name | Affiliation | Role |
|---|---|---|
| Gunnar Tepe, MD | Institut fĂĽr Diagnostische und Interventionelle Radiologie, RoMed Klinikum Rosenheim | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Cardiologisches Centrum Bethanien | Frankfurt | Germany | ||||
| Asklepios Kliniken Hamburg GmbH |
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Defined as a composite rate of all-cause death, target limb major amputation and CD-TLR
| 12 months |
| Major adverse event (MAE) rate at 6,12, and 24 months post index procedure | Defined as a composite rate of all-cause death, target limb major amputation and CD-TLR | 24 months |
| Rate of CD-TLR at 6, 12 and 24 months | Rate of CD-TLR | 6 months |
| Rate of CD-TLR at 6, 12 and 24 months | Rate of CD-TLR | 12 months |
| Rate of CD-TLR at 6, 12 and 24 months | Rate of CD-TLR | 24 months |
| Patency rate at 6, 12 and 24 months, defined as the presence of target lesion flow (absence of occlusion or no flow) as determined by Duplex Ultrasound (DUS) and freedom from CD-TLR | Patency rate | 6 months |
| Patency rate at 6, 12 and 24 months, defined as the presence of target lesion flow (absence of occlusion or no flow) as determined by Duplex Ultrasound (DUS) and freedom from CD-TLR | Patency rate | 12 months |
| Patency rate at 6, 12 and 24 months, defined as the presence of target lesion flow (absence of occlusion or no flow) as determined by Duplex Ultrasound (DUS) and freedom from CD-TLR | Patency rate | 24 months |
| Rate of procedural complications defined as occurrence of all-cause death, stroke, myocardial infarction, emergent surgical revascularization, significant distal embolization in target limb, or thrombosis of target vessel through the end of the procedure | Rate of procedural complications | through study completion, approximately 5 years |
| Rate of device or procedure related death at 30 days | Rate of device or procedure related death | 30 days |
| Rate of major target limb amputation at 6 months post-procedure | Rate of major target limb amputation | 6 months |
| Rate of major target limb amputation at 12 months post-procedure | Rate of major target limb amputation | 12 months |
| Rate of major target limb amputation at 24 months post-procedure | Rate of major target limb amputation | 24 months |
| Rate of clinically driven target vessel revascularization through 6 months | Rate of clinically driven target vessel revascularization | 6 months |
| Rate of clinically driven target vessel revascularization through 12 months | Rate of clinically driven target vessel revascularization | 12 months |
| Rate of clinically driven target vessel revascularization through 24 months | Rate of clinically driven target vessel revascularization | 24 months |
| Lesion success: | Achievement of a final in-lesion residual diameter stenosis of <50% (as determined by the angiographic core laboratory), using allowed pretreatment devices after guidewire passage through the lesion | Through study completion, approximately 5 years |
| Technical success: | Achievement of a final in-lesion residual diameter stenosis of <50% (as determined by the angiographic core laboratory), using the Stellarex 0.014" Drug-Coated Balloon without a device malfunction after a guidewire passage through the l | Through study completion, approximately 5 years |
| Change in waveforms/TcPO2 from pre-procedure to 30 days | Change in waveforms/TcPO2 from pre-procedure | 30 days |
| Change in waveforms/TcPO2 from pre-procedure to 6 months | Change in waveforms/TcPO2 from pre-procedure | 6 months |
| Change in waveforms/TcPO2 from pre-procedure to 12 months | Change in waveforms/TcPO2 from pre-procedure | 12 months |
| Change in waveforms/TcPO2 from pre-procedure to 24 months | Change in waveforms/TcPO2 from pre-procedure | 24 months |
| Change in ankle-brachial index (ABI) from pre-procedure to 30 days | Change in ankle-brachial index (ABI) from pre-procedure | 30 days |
| Change in ankle-brachial index (ABI) from pre-procedure to 6 months | Change in ankle-brachial index (ABI) from pre-procedure | 6 months |
| Change in ankle-brachial index (ABI) from pre-procedure to 12 months | Change in ankle-brachial index (ABI) from pre-procedure | 12 months |
| Change in ankle-brachial index (ABI) from pre-procedure to 24 months | Change in ankle-brachial index (ABI) from pre-procedure | 24 months |
| Change in toe pressures (TP) from pre-procedure to 30 days | Change in toe pressures (TP) from pre-procedure | 30 days |
| Change in toe pressures (TP) from pre-procedure to 6 months | Change in toe pressures (TP) from pre-procedure | 6 months |
| Change in toe pressures (TP) from pre-procedure to 12 months | Change in toe pressures (TP) from pre-procedure | 12 months |
| Change in toe pressures (TP) from pre-procedure to 24 months | Change in toe pressures (TP) from pre-procedure | 24 months |
| Change in Rutherford-Becker Classification (RCC) from pre-procedure to 30 days | Change in Rutherford-Becker Classification (RCC) from pre-procedure | 30 days |
| Change in Rutherford-Becker Classification (RCC) from pre-procedure to 6 months | Change in Rutherford-Becker Classification (RCC) from pre-procedure | 6 months |
| Change in Rutherford-Becker Classification (RCC) from pre-procedure to 12 months | Change in Rutherford-Becker Classification (RCC) from pre-procedure | 12 months |
| Change in Rutherford-Becker Classification (RCC) from pre-procedure to 24 months | Change in Rutherford-Becker Classification (RCC) from pre-procedure | 24 months |
| Change in EQ-5D from pre-procedure to 30 days | Change in EQ-5D-5L (EuroQual-5 Dimension scale set and Visual Analog Scale score) from pre-procedure. Dimension score reporting will be determined at time of reporting and VAS score will be reported based on subject indicated scale from 0 to 100, where higher scores indicate positive outcome improvement. | 30 days |
| Change in EQ-5D from pre-procedure to 6 months | Change in EQ-5D-5L (EuroQual-5 Dimension scale set and Visual Analog Scale score) from pre-procedure. Dimension score reporting will be determined at time of reporting and VAS score will be reported based on subject indicated scale from 0 to 100, where higher scores indicate positive outcome improvement. | 6 months |
| Change in EQ-5D from pre-procedure to 12 months | Change in EQ-5D-5L (EuroQual-5 Dimension scale set and Visual Analog Scale score) from pre-procedure. Dimension score reporting will be determined at time of reporting and VAS score will be reported based on subject indicated scale from 0 to 100, where higher scores indicate positive outcome improvement. | 12 months |
| Change in EQ-5D from pre-procedure to 24 months | Change in EQ-5D-5L (EuroQual-5 Dimension scale set and Visual Analog Scale score) from pre-procedure. Dimension score reporting will be determined at time of reporting and VAS score will be reported based on subject indicated scale from 0 to 100, where higher scores indicate positive outcome improvement. | 24 months |
| In RCC 5 subjects, percentage of wounds healed from baseline to 30 days post-procedure as reported by the Investigator at the Investigative site | In RCC 5 subjects, percentage of wounds healed from baseline | 30 days |
| In RCC 5 subjects, percentage of wounds healed from baseline to 6 months post-procedure as reported by the Investigator at the Investigative site | In RCC 5 subjects, percentage of wounds healed from baseline | 6 months |
| In RCC 5 subjects, percentage of wounds healed from baseline to 12 months post-procedure as reported by the Investigator at the Investigative site | In RCC 5 subjects, percentage of wounds healed from baseline | 12 months |
| Hamburg |
| Germany |
| Klinik Immenstadt, Herz und GefaSzentrum Immenstadt | Immenstadt im Allgäu | Germany |
| Universitatsmedizin der Johannes Gutenberg-Universitat Mainz | Mainz | Germany |
| RoMed Klinikum Rosenheim | Rosenheim | Germany |
| Albert Schweitzer Hospital | Dordrecht | Netherlands |
| St. Antonius Hospital | Nieuwegein | Netherlands |
| Cambridge University Hospital | Cambridge | United Kingdom |
| Guys and St. Thomas Hospital | London | United Kingdom |
| The Royal Free Hospital | London | United Kingdom |
| ID | Term |
|---|---|
| D058729 | Peripheral Arterial Disease |
| D000089802 | Chronic Limb-Threatening Ischemia |
| D007383 | Intermittent Claudication |
| ID | Term |
|---|---|
| D050197 | Atherosclerosis |
| D001161 | Arteriosclerosis |
| D001157 | Arterial Occlusive Diseases |
| D014652 | Vascular Diseases |
| D002318 | Cardiovascular Diseases |
| D016491 | Peripheral Vascular Diseases |
| D002908 | Chronic Disease |
| D020969 | Disease Attributes |
| D010335 | Pathologic Processes |
| D013568 | Pathological Conditions, Signs and Symptoms |
| D007511 | Ischemia |
| D012816 | Signs and Symptoms |
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