- Article
OPEN ACCESS ARTICLE
- R. Scott Turner, MD, PhD,
- Ronald G. Thomas, PhD,
- Suzanne Craft, PhD,
- Christopher H. van Dyck, MD,
- Jacobo Mintzer, MD,
- Brigid A. Reynolds, NP,
- James B. Brewer, MD, PhD,
- Robert A. Rissman, PhD,
- Rema Raman, PhD,
- Paul S. Aisen, MD;
- For the Alzheimer's Disease Cooperative Study
- Correspondence to Dr. Turner: rst36@georgetown.edu
-
10.1212/WNL.0000000000002035Neurology
- Free via Open Access: OA
- Abstract
- Full Text (PDF)
- Also available:
- Data Supplement
- Coinvestigators
Abstract
Objective: A
randomized, placebo-controlled, double-blind, multicenter 52-week phase 2
trial of resveratrol in individuals with mild
to moderate Alzheimer disease (AD) examined its
safety and tolerability and effects on biomarker (plasma Aβ40 and Aβ42,
CSF
Aβ40, Aβ42, tau, and phospho-tau 181) and
volumetric MRI outcomes (primary outcomes) and clinical outcomes
(secondary outcomes).
Methods:
Participants (n = 119) were randomized to placebo or resveratrol 500 mg
orally once daily (with dose escalation by 500-mg
increments every 13 weeks, ending with 1,000 mg
twice daily). Brain MRI and CSF collection were performed at baseline
and
after completion of treatment. Detailed
pharmacokinetics were performed on a subset (n = 15) at baseline and
weeks 13, 26,
39, and 52.
Results: Resveratrol
and its major metabolites were measurable in plasma and CSF. The most
common adverse events were nausea, diarrhea,
and weight loss. CSF Aβ40 and plasma Aβ40 levels
declined more in the placebo group than the resveratrol-treated group,
resulting
in a significant difference at week 52. Brain
volume loss was increased by resveratrol treatment compared to placebo.
Conclusions:
Resveratrol was safe and well-tolerated. Resveratrol and its major
metabolites penetrated the blood–brain barrier to have
CNS effects. Further studies are required to
interpret the biomarker changes associated with resveratrol treatment.
Classification of evidence:
This study provides Class II evidence that for patients with AD
resveratrol is safe, well-tolerated, and alters some AD biomarker
trajectories. The study is rated Class II
because more than 2 primary outcomes were designated.
- Received January 6, 2015.
- Accepted in final form June 19, 2015.
- © 2015 American Academy of Neurology
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