Abstract

Intravenous (IV) administration of tissue plasminogen activator (tPA) is an effective therapy for acute stroke when treatment is begun within 3 hours of symptom onset. The success of tPA therapy is attributed to the medication's ability to open occluded cerebral arteries before irreversible brain injury has occurred. Benefits of tPA, or any other stroke therapy, have not been clearly established for patients treated between 3-6 hours after stroke onset, a time period when a substantial number of patients present for evaluation. We believe this therapeutic failure has occurred because some patients treated 3-6 hours after symptom onset have already sustained severe, irreversible brain injury and others have undergone spontaneous recanalization of their occluded arteries. The results of our previous pilot trial, DEFUSE 1, indicate that baseline MRI profiles appear to differentiate patient subgroups that can benefit substantially from 3-6 hour IV tPA therapy from subgroups that do not benefit. DEFUSE 2 is an international, multicenter, open-label, pilot study of 100 patients who present 3-6 hours after stroke onset. Based on the MRI profiles identified in DEFUSE 1, patients will be treated with IV tPA. Two follow-up MRI scans will assess whether early reperfusion and/or recanalization occurs and establish the final infarct volume. The primary outcome assessment is based on the degree of neurologic improvement at 30 days. We hope to a) validate the results of the DEFUSE 1 study by confirming that specific MRI profiles are predictive of the clinical response to early reperfusion, and b) demonstrate that an automated analysis of DWI and PWI data can be performed quickly and accurately at multiple clinical sites utilizing MRI scanners from different manufacturers.

Public Health Relevance

The key objective of DEFUSE 1 and 2 is to obtain sufficient preliminary data to optimally design a randomized trial that will assess the benefits of reperfusion therapy, administered 3-6 hrs after stroke symptom onset, using baseline MRI findings to select patents who are likely to have a robust clinical benefit from early reperfusion. We believe that the DEFUSE 2 study will clarify the key mediators of clinical outcomes in acute stroke patients and lead to a randomized trial that will demonstrate the efficacy of IV tPA therapy for a large population of patients who are currently ineligible for treatment. The key objective of DEFUSE 2 is to obtain sufficient preliminary data to optimally design a definitive study to assess the risks and benefits of treatment of stroke patients with a clot dissolving medication beyond the current 3 hour time window. We believe that the DEFUSE 2 study will clarify that specific MRI findings can identify patients who benefit from therapy 3-6 hours after symptom onset. These findings will eventually lead to effective therapies for a large population of stroke patients who are currently ineligible for treatment and substantially reduce stroke-related disability.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS039325-04A2
Application #
7524998
Study Section
National Institute of Neurological Disorders and Stroke Initial Review Group (NSD)
Program Officer
Moy, Claudia S
Project Start
1999-12-01
Project End
2011-08-31
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
4
Fiscal Year
2009
Total Cost
$1,591,334
Indirect Cost

  Institution

Name
Stanford University
Department
Neurology
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Wouters, Anke; Dupont, Patrick; Christensen, Soren et al. (2016) Association Between Time From Stroke Onset and Fluid-Attenuated Inversion Recovery Lesion Intensity Is Modified by Status of Collateral Circulation. Stroke 47:1018-22
Tu, Hans T H; Campbell, Bruce C V; Christensen, Soren et al. (2015) Worse stroke outcome in atrial fibrillation is explained by more severe hypoperfusion, infarct growth, and hemorrhagic transformation. Int J Stroke 10:534-40
Yassi, Nawaf; Churilov, Leonid; Campbell, Bruce C V et al. (2015) The association between lesion location and functional outcome after ischemic stroke. Int J Stroke 10:1270-6
Wheeler, Hayley M; Mlynash, Michael; Inoue, Manabu et al. (2015) The growth rate of early DWI lesions is highly variable and associated with penumbral salvage and clinical outcomes following endovascular reperfusion. Int J Stroke 10:723-9
Purushotham, Archana; Campbell, Bruce C V; Straka, Matus et al. (2015) Apparent diffusion coefficient threshold for delineation of ischemic core. Int J Stroke 10:348-53
Mishra, Nishant K; Albers, Gregory W; Christensen, Søren et al. (2014) Comparison of magnetic resonance imaging mismatch criteria to select patients for endovascular stroke therapy. Stroke 45:1369-74
Lemmens, Robin; Christensen, Søren; Straka, Matus et al. (2014) Patients with single distal MCA perfusion lesions have a high rate of good outcome with or without reperfusion. Int J Stroke 9:156-9
Inoue, Manabu; Mlynash, Michael; Straka, Matus et al. (2013) Clinical outcomes strongly associated with the degree of reperfusion achieved in target mismatch patients: pooled data from the Diffusion and Perfusion Imaging Evaluation for Understanding Stroke Evolution studies. Stroke 44:1885-90
Campbell, Bruce C V; Christensen, Søren; Parsons, Mark W et al. (2013) Advanced imaging improves prediction of hemorrhage after stroke thrombolysis. Ann Neurol 73:510-9
Wheeler, Hayley M; Mlynash, Michael; Inoue, Manabu et al. (2013) Early diffusion-weighted imaging and perfusion-weighted imaging lesion volumes forecast final infarct size in DEFUSE 2. Stroke 44:681-5

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