grant

FVIIa for Acute hemorrhagic Stroke Administered at Earliest Time (FASTEST) Trial

Organization UNIVERSITY OF CINCINNATILocation CINCINNATI, UNITED STATESPosted 1 Mar 2020Deadline 31 Dec 2026
NIHUS FederalResearch GrantFY2026Activated Blood Coagulation Factor VIIActivated Factor VIIAcuteAgeAlteplaseAmerican Heart AssociationApoplexyAustraliaBleedingBlood PressureBrain IschemiaBrain Vascular AccidentBrain hemorrhageBrain imagingCAT scanCT X RayCT XrayCT imagingCT scanCanadaCardiac infarctionCaringCerebral Brain HemorrhageCerebral HemorrhageCerebral InfarctionCerebral Parenchymal HemorrhageCerebral StrokeCerebral hemisphere hemorrhageCerebrovascular ApoplexyCerebrovascular StrokeCerebrum HemorrhageCessation of lifeCoagulation Factor VIIaComputed TomographyCountryDeathDoseDouble-Blind MethodDouble-Blind StudyDouble-BlindedDouble-Masked MethodDouble-Masked StudyDropsyDrugsEdemaEmbolismEmbolusEventFactor VIIaFavorable Clinical OutcomeGeneralized GrowthGermanyGlasgow Coma ScaleGoalsGrowthGuidelinesHeadHemorrhageHospitalsHourHydropsImageInformed ConsentInstitutionIntracerebral HemorrhageIschemiaIschemic EncephalopathyIschemic StrokeJapanJordanMeasurementMeasuresMedicalMedicationMyocardial InfarctMyocardial InfarctionNINDSNational Institute of Neurological Diseases and StrokeNational Institute of Neurological Disorders and StrokeOutcome MeasureParticipantPatient RecruitmentsPatient SelectionPatient outcomePatient-Centered OutcomesPatient-Focused OutcomesPatientsPharmaceutical PreparationsPhasePhonePhysiologicPhysiologicalPlacebosPrincipal InvestigatorProliferatingPublishingRandomizedRecombinant Tissue Plasminogen ActivatorRecombinantsReportingSham TreatmentSiteSpainStrokeT-Plasminogen ActivatorTelephoneTestingTimeTissue Activator D-44Tissue GrowthTissue Plasminogen ActivatorTissue-Type Plasminogen ActivatorTomodensitometryTriageUnited KingdomX-Ray CAT ScanX-Ray Computed TomographyX-Ray Computerized TomographyXray CAT scanXray Computed TomographyXray computerized tomographyagesarmbleeding in brainblood lossbrain attackbrain visualizationcardiac infarctcare servicescare systemscatscancerebral infarctcerebral vascular accidentcerebrovascular accidentcomputed axial tomographycomputer tomographycomputerized axial tomographycomputerized tomographycoronary attackcoronary infarctcoronary infarctiondrug/agentefficacy outcomesheart attackheart infarctheart infarctionhemorrhagic strokeimagingimproved outcomeintraventricular hemorrhagemeasurable outcomenon-contrast CTnoncontrast CTnoncontrast computed tomographyontogenyoutcome measurementoutcome predictionparticipant recruitmentpatient oriented outcomesprimary outcomepulmonaryrandomisationrandomizationrandomized, clinical trialsrandomly assignedrecruitsafety outcomessham therapystroke patientstrokedstrokest-PAtreatment guidelines
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Full Description

Project Summary
Recombinant Factor VIIa (rFVIIa) for Acute hemorrhagic Stroke Administered at Earliest Time (FASTEST) Trial
is a randomized, double-blind, controlled global trial of rFVIIa plus best standard therapy vs. best standard
therapy alone for patients with intracerebral hemorrhage (ICH). Our central hypothesis is that treatment with
rFVIIa within two hours of onset in appropriately selected patients with spontaneous ICH improves outcome as
measured by the ordinal distribution of the modified Rankin Scale (mRS) at 90 days, as compared to placebo.
We will test our hypothesis in 860 patients recruited at 100 hospital sites and at least 15 mobile stroke units
(MSUs) within the NINDS StrokeNet (70 sites) and key global institutions (30 sites) with large volumes of
patients with ICH and ability to treat within 2 hours of onset. Participating countries include the U.S., Canada,
United Kingdom, Germany, Spain, Japan, and Australia. We will include subjects with a volume of ICH < 60 cc,
no intraventricular hemorrhage (IVH) or a small volume of IVH (IVH score ≤ 7), age ≤ 80, GCS ≥ 8, and treated
within 120 minutes from last known normal. To minimize time-to-treatment, the study will use exception from
informed consent and MSUs with a goal of ½ of patients treated within 90 minutes as accomplished in the
NINDS t-PA trials. We will recruit the 860 patients over 3 1/2 years and randomize them in a double-blinded
fashion to rFVIIa 80 micrograms/kg dose (maximum 8mg dose) or placebo. Subjects in both arms will receive
best medical therapy as per published AHA Guidelines for ICH, including a target blood pressure of 140 mm
Hg. The primary efficacy outcome measure is the ordinal distribution of the mRS at 90 days. Primary safety
outcomes will include ischemic events (cerebral infarction, myocardial infarction, and pulmonary embolus)
within 4 days of study medication. To measure growth of ICH and IVH, all subjects will have baseline non-
contrast CT and at 24 hours. Centralized volumetric measurements of ICH, IVH, and edema will be done for
both time-points. The overall principal investigators (PIs) for the Trial include Joseph Broderick, James Grotta,
Andrew Naidech, and Jordan Elm (primary statistical PI) as well as PIs for each participating non-U.S. country.
In summary, the goal of FAST is to find the first scientifically proven treatment for acute ICH.

Grant Number: 5U01NS110772-05
NIH Institute/Center: NIH
Principal Investigator: Joseph Broderick

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