Study to Determine The Effect of a Drug Called Neupogen on Stroke Recovery
NCT ID: NCT00809549
Last Updated: 2012-07-13
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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UNKNOWN
PHASE1
20 participants
INTERVENTIONAL
2006-07-31
2013-04-30
Brief Summary
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2. Increasing the number of circulating precursors will improve in regeneration of damaged brain following ischemic stroke.
Detailed Description
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Underlying this work are the following considerations:
* Currently the clinical and functional outcomes following ischemic strokes are poor and require new treatment strategies.
* G-CSF administration is a well established routine treatment for the mobilization of hematopoietic and endothelial precursors from the bone marrow into the circulation.
* Acute ischemia locally increases factors that direct circulating bone marrow derived cells to home to these sites of injury.
* Evidence exists that bone marrow derived cells are able to repopulate different tissues including those of the CNS.
* Acute ischemic injury to the central nervous system provides a milieu for the regeneration of neural tissue.
Conditions
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Keywords
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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Normal Saline
Filgrastim
10 ug/kg sc once daily x 4 days. Repeated once, 6 weeks later.
Filgrastim
Filgrastim
10 ug/kg sc once daily x 4 days. Repeated once, 6 weeks later.
Interventions
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Filgrastim
10 ug/kg sc once daily x 4 days. Repeated once, 6 weeks later.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Patient is of either gender
* The qualifying stroke is ischemic with a total NIH Stroke Score less than 18.
* The stroke involves the non-dominant hemisphere including the cerebral cortex and results in hemiparesis. The inclusion of sub-cortical strokes will be permitted if the size is of 3 cm or greater. Patients suffering strokes involving the dominant hemisphere resulting in mild dysphasia are also eligible.
* The stroke is classified as a partial anterior cerebral syndrome by the Oxfordshire Criteria.
* NIHSS at baseline evaluation with:
\*Level of consciousness is not impaired as defined by an NIHSS between 0 and 1 on question 1a and
* Hemiparesis as defined by
* an NIHSS between 1 and 4 on questions 5 and/or
* an NIHSS between 1 and 4 on questions 6.
* Be able to start the experimental treatment a minimum of 3 days and a maximum of 10 days after the initial presentation with the stroke,
* Patient or surrogate gives informed consent,
* The patient is fluent in either French or English.
Exclusion Criteria
* Patients with a pre-morbid modified Rankin score \> 2 (Appendix 3b),
* Patients with pre-morbid dementia by DSM-IV criteria.
* Patients with a known allergic reaction to G-CSF or a component of G-CSF.
* Patients with one or more significant co-morbidities expected to limit lifespan to less than 12 months. Examples include but are not limited to:
* \> CHF Class II NYHA
* Known prior or ongoing malignancy except non-melanomatous skin cancer.
* Acute or chronic infections (HIV, TB, etc.. )
* Other significant cardiac, renal, hepatic or pulmonary dysfunction.
* Patients with organ dysfunction that would preclude tests required for this study. Examples include but are not limited to:
\*Serum Cr \> 200 μmol/L that would prevent administration of contrast dye.
* Patients with a known history of bone marrow dysfunction, such as myeloid leukemia or myeloproliferative state that would prevent treatment with G-CSF.
* Patients with metal implants that would preclude MRI examination including but not limited to patients with
* pacemakers,
* ear implants, and
* aneurysm brain clips.
* Patients with:
* a history compatible with a thrombophilic state or
* with a pre-existing known thrombophilic state.
* Patient unwilling or unable to comply with trial requirements.
* Patients with an ongoing history of illicit drug use.
* Female patients of child-bearing potential.
* Patients exposed to other investigational drugs in the last 3 months.
* Patients with known or suspected sickle cell disease,
* Patients with splenic enlargement or an illness that results in splenic enlargement (For example, but not limited to myeloproliferative syndromes, hairy cell leukaemia, malaria, hepatic cirrhosis…),
* Patients with an ongoing history of alcohol abuse,
* Patients with a known or suspected history of allergy to intravenous contrast agents used for CT scans,
* Patients that have received a chemotherapy agent within the previous 5 years (For example, but not limited to cyclophosphamide, anthracycline, methotrexate, fluorouracil…)
* Patients that have received a therapy within the previous 5 years that interferes with hematopoiesis or circulating blood cells (For example, but not limited to Lithium, Campath….)
* Patients that have received a cytokine within the last 6 months or are currently receiving a cytokine treatment (For example, but not limited to Erythropoietin, Granulocyte Macrophage Colony Stimulating Factor, Keratinocyte Growth Factor, Kit Ligand…)
45 Years
85 Years
ALL
No
Sponsors
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Ottawa Hospital Research Institute
OTHER
Responsible Party
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Principal Investigators
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Michael Sharma, MD
Role: PRINCIPAL_INVESTIGATOR
The Ottawa Hospital
Locations
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The Ottawa Hospital
Ottawa, Ontario, Canada
Sunnybrook Health Sciences Centre
Toronto, Ontario, Canada
Countries
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Other Identifiers
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2006076-01H
Identifier Type: -
Identifier Source: org_study_id