Title
A Dose Escalation and Safety Study of Plasmin (Human) In Acute Lower Extremity Native Artery or Bypass Graft Occlusion
A Sequential Phase I/II Dose Escalation and Dose Selection Safety Study of Regional Intra-thrombus Plasmin (Human) Infusion In Acute Lower Extremity Native Artery or Bypass Graft Occlusion
Phase
Phase 1Lead Sponsor
GrifolsStudy Type
InterventionalStatus
Completed No Results PostedIndication/Condition
Arterial Occlusive DiseasesIntervention/Treatment
fibrinolysin, human ...Study Participants
83The purpose of this study is to evaluate the safety of increasing doses of intra-thrombus Plasmin (Human) in acute peripheral arterial occlusion (aPAO). The ability of these Plasmin doses to dissolve the clots will be estimated by arteriography.
There is an unmet need for proven thrombolytic agent in acute peripheral arterial occlusion (aPAO). The current assortment of plasminogen activators are slow to dissolve clots in the leg, and may lead to bleeding complications. Plasmin is a direct thrombolytic that may act more quickly when infused directly into the clot and thus assist in restoring blood flow to the leg. There is a large reserve in blood alpha-2 antiplasmin in the blood to rapidly inactivate Plasmin outside of the clot. Plasmin has the potential for an improved bleeding risk profile in aPAO.
Plasmin (Human) 25 mg delivered via an infusion catheter into the thrombus over approximately 5 hours.
Plasmin (Human) 50 mg delivered via an infusion catheter into the thrombus over approximately 5 hours.
Plasmin (Human) 75 mg delivered via an infusion catheter into the thrombus over approximately 5 hours.
Plasmin (Human) 100 mg
Plasmin (Human) 125 mg delivered via an infusion catheter into the thrombus over approximately 5 hours.
Plasmin (Human) 150 mg delivered via an infusion catheter into the thrombus over approximately 5 hours.
Plasmin (Human) 175 mg delivered via an infusion catheter into the thrombus over approximately 5 hours.
Inclusion Criteria: Age ≥ 18 years. Women of childbearing potential must use adequate contraception for the duration of the study and must have a negative pregnancy test prior to study entry. Unilateral limb ischemia: SVS acute ischemia Category I or IIa. Onset of symptoms </= 14 days. Thrombosed (non-embolic) infrainguinal graft (synthetic, autologous, or single outflow composite) or infrainguinal native artery. For native arteries, only occlusions of ≥ 10 cm in length are eligible. Diagnosis of occlusive thrombus in the graft or artery by arteriography after Informed Consent is obtained. Ability to traverse the thrombus with a guidewire. Signed informed consent prior to study entry. Exclusion Criteria: Clinical evidence of significant disease that may interfere with the patient successfully completing the trial. Women who are pregnant or lactating, or first 10 days post-partum. Previous hemorrhagic stroke at any time. Thrombotic or embolic stroke or cerebrovascular events (including transient ischemic attack (TIA)) within one year. Intracranial or spinal neuro-surgery, or severe intracranial trauma in the last 3 months. Major surgery, organ biopsy, or major trauma within the last 10 days. Lumbar puncture or non-compressible arterial puncture in the last 10 days. Intra-ocular surgery within the last 10 days. Current bleeding diathesis. Active gastrointestinal or organ bleeding. Minor bleeding such as normal menses, cystitis, or minor hemorrhoidal bleeding are not exclusions. Uncontrolled arterial hypertension, defined as a systolic blood pressure > 180 mmHg or diastolic blood pressure > 110 mmHg. Known intracranial neoplasm, aneurysm, or arterio-venous malformation. Platelet count < 75 x 10e9/L. Occlusion of a graft within 6 months of placement. Medically unable to tolerate an open vascular procedure. Known prothrombotic condition. Hemoglobin <10.0 g/dL Impaired renal function or renal disease that constitutes a contraindication to contrast angiography, including creatinine > 2.0 mg/dL or subjects on renal dialysis. Treatment with a glycoprotein IIb/IIIa class of platelet inhibitor within the past 5 days, for example, abciximab (ReoPro®), eptifibatide (Integrilin®) or tirofiban (Aggrastat®). Treatment with warfarin (Coumadin®) and with an INR of >1.7 (elevated INR at screening may be corrected prior to study enrollment.)