Cerebrovascular Accident Clinical Trial
Official title:
ReoPro Retavase Reperfusion of Stroke Safety Study - Imaging Evaluation
This study will evaluate the safety and effectiveness of two types of blood thinners,
abciximab (ReoPro) and reteplase (Retavase) for restoring normal brain blood flow after
ischemic stroke (stroke resulting from a blood clot in the brain).
The only therapy approved by the Food and Drug Administration to treat ischemic stroke is
the clot buster drug rt-PA. This treatment, however, is effective only if begun within 3
hours of onset of the stroke and most patients do not get to the hospital early enough to
benefit from it. There is thus a pressing need to develop effective stroke treatments that
can be initiated more than 3 hours after onset.
Patients between 18 and 80 years of age who have experienced a mild or moderate acute stroke
between 3 and 24 hours before starting study drugs may be eligible for this study.
Candidates will be screened with a physical examination, blood tests and a magnetic
resonance imaging (MRI) scan (if an MRI was not done during the stroke evaluation).
All participants will receive ReoPro. Some will also receive Retavase, which may boost the
effectiveness of ReoPro. Retavase is administered in a single dose through a needle in the
vein over 2 minutes. ReoPro is infused into the vein over 12 hours. Patients will be
monitored with physical examinations, blood tests, computed tomography (CT) scans, and three
or four MRI scans of the brain to evaluate both the response to treatment and side effects
of the drugs. An MRI scan will be done 24 hours, 5 days and 30 days after starting the study
medication, and possibly during screening for this study.
CT involves the use of specialized x-rays to obtain images of the brain. The patient lies
still in the scanner for a short time while the X-ray images are formed. MRI uses a strong
magnetic field and radio waves to demonstrate structural and chemical changes in tissue. MRI
is more sensitive than x-ray in evaluating acute stroke. The patient lies on a table in a
metal cylinder (the scanner) while the pictures are being taken. During part of the MRI, a
medicine called gadolinium contrast is injected in a vein. This medicine brightens the
images, creating better pictures of the blood flow.
Objectives: This is a clinical trial to determine an acceptable dose of reteplase in
combination with a fixed dose of abciximab for ischemic stroke 3-24 hours from onset.
Study Population: Patients will be selected by criteria to minimize likelihood of toxicity
and maximize likelihood of response. These criteria include age 18-80 years old, acute
ischemic stroke of moderate severity (NIH Stroke Scale less than or equal to 16 and lesion
volume on diffusion MRI less than approximately one third of the volume of the middle
cerebral artery territory), positive MRI evidence of hypoperfusion corresponding to the
acute stroke symptoms, no MRI evidence of chronic micro-hemorrhages, and no other clinical,
radiological or laboratory features associated with risk of hemorrhage with thrombolytic
therapy.
Design: The study is open-label, dose escalation, safety and proof of principle study of the
combination of intravenous abciximab and reteplase. A fixed dose of abciximab will be used
in all patients: 0.25 mg/kg bolus (to a maximum of 30 mg) followed by a 0.125
microgram/kg/minute infusion (to a maximum of 10.0 microgram/minute) for 12 hours. The five
dosing groups for the reteplase dose are 0 U, 2.5 U, 5.0 U, 7.5 U, and 10.0 U. A maximum of
72 patients will be treated using an adaptive statistical design, in which data on both the
response and toxicity will be used to determine the dose for subsequent patients, thereby
minimizing exposure to either ineffective or toxic doses. Non-investigational patient
management will be standardized across all patients according to the NIH Stroke Center
Clinical Care Pathway.
Outcome Measures: The primary efficacy endpoint for response will be reperfusion by MRI 24
hours after start of therapy. The primary safety endpoint for determination of toxicity will
be any one of the following: symptomatic intracranial hemorrhage (ICH), major systemic
hemorrhage, or other serious adverse event related to study drug administration, including
death, within 48 hours from start of therapy. The maximum acceptable rate of toxicity will
be 10% of patients treated at any dose level and the minimum acceptable rate of response
will be 50% of patients treated at any dose level. The outcomes will be monitored by a Data
and Safety Monitoring Committee, which will have the authority to stop or recommend
modifications of the trial for safety concerns. Other clinical outcome variables and imaging
variables will be recorded and analyzed in secondary and exploratory analyses. If an
acceptable dose is identified, then that will be investigated in a subsequent randomized
placebo-controlled trial.
;
Primary Purpose: Treatment
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