Alzheimer's Disease Clinical Trial
Official title:
Efficacy and Safety of Filgrastim as a Pro‐Cognitive Agent in Alzheimer's Disease
Filgrastim (G-CSF) is widely used for treatment of patients who have a deficiency of white blood cells. It is also routinely used to stimulate and mobilize stem/progenitor cells for bone marrow transplantation. In studies of thousands of healthy donor subjects treated with G-CSF, the side-effects profile has been reported to be mild and reversible. Currently, G-CSF is under investigation in clinical trials in Germany and the US that aim to enhance recovery from strokes and heart attacks. In animal studies, G-CSF has been observed to improve cognitive performance and to markedly reduce amyloid deposition in hippocampus and entorhinal cortex in a mouse model of Alzheimer's Disease (AD). Since this drug is being used safely in many people throughout the world, the investigators hypothesize that it will also be safe to give to patients with Alzheimer's disease and that it may improve some aspects of memory and thinking. The present pilot study has two goals or objectives: 1) to investigate the effects of a five day schedule of Filgrastim administration on cognitive function and 2) to assess its tolerability and safety in a small group (12 patients) with mild to moderate stage AD. Patients who are eligible for the study will be randomly assigned to one of two groups (n=6 per group). One group will receive a five-day course of Filgrastim injections and the other group of subjects will receive vehicle injections (solution without drug). At the end of the first phase of the study (week 8), the groups will cross over to receive either vehicle or Filgrastim as appropriate. In this way all subjects will have received the active medication by the end of the study. After the study is finished the investigators should know whether or not Filgrastim improves some aspects of thinking and memory. And the investigators should know whether or not it is safe to give this medication to patients with Alzheimer's disease. To ensure that the drug is safe, a Safety Monitoring Committee will oversee the entire study. They will review all laboratory data, including complete blood counts, serum chemistry, EKGs and adverse events.
The study was originally designed to have two arms (GCSF first followed by placebo= Arm 1;
placebo followed by GCSF=Arm2). Total length of study for each subject was 14 weeks, with
crossover on week 7.
Linear regression models could not be used because of the small number of subjects; n = 5 in
the first Arm who received G-CSF before crossover to the placebo phase and n = 3 in Arm 2
(who received placebo first before crossover to the G-CSF treatment phase). The general rule
for the sample size required for regression analysis is n = 15 per covariate. Therefore,
comparison of the final cognitive scores on visit 5 (week 14) were compared to scores at
baseline (visit 1) for all subjects (n = 8) using the Wilcoxon signed rank test. Plasma
cytokine changes were plotted to compare effects following G-CSF to that following placebo,
regardless of the order of treatment. Wilcoxon sum rank test was used to test differences
between G-CSF treatment and placebo treatment at specific intervals after treatment.
Statistical Package for the Social Sciences (SPSS Version 19) was used for all data
analysis.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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