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Article type: Research Article
Authors: Bennett, Jamesa; b; * | Burns, Jeffreyc | Welch, Paulc | Bothwell, Rebeccac
Affiliations: [a] Virginia Commonwealth University Parkinson’s Center, Richmond, VA, USA | [b] Neurodegeneration Therapeutics, Inc., Charlottesville, VA, USA | [c] University of Kansas School of Medicine Alzheimer’s Disease Center, Kansas City, KS, USA
Correspondence: [*] Correspondence to: James P. Bennett, Jr., MD, PhD, Neurodegeneration Therapeutics, Inc., 3050A Berkmar Drive, Charlottesville, VA 22901, USA. Tel.: +1 434 529 6457; Fax: +1 434 529 6458; E-mail: aging.mitochondria@gmail.com.
Abstract: Alzheimer’s disease (AD) is an aging-related, degenerative brain disease of adults. Most (∼95%) of AD occurs sporadically and is associated with early-appearing deficits in brain regional glucose uptake, changes in cerebrospinal fluid (CSF) AD-related proteins, regional brain atrophy, and oxidative stress damage. We treated mild-moderate AD individuals with R(+)-pramipexole-dihydrochloride (R(+)PPX), a neuroprotective, lipophilic-cation, free-radical scavenger that accumulates into brain and mitochondria. 19 subjects took R(+)PPX twice a day in increasing daily doses up to 300 mg/day under a physician-sponsor IND (60,948, JPB), IRB-approved protocol and quarterly external safety committee monitoring. 15 persons finished and contributed baseline and post-treatment serum, lumbar spinal fluid, brain 18F-2DG PET scans, and ADAS-Cog scores. ADAS-Cog scores did not change (n = 1), improved (n = 2), declined 1–3 points (n = 5), or declined 4–13 points (n = 8) over 6 months of R(+)PPX treatment. Serum PPX levels were not related to changes in ADAS-Cog scores. Fasting AM serum PPX levels at 6 months varied considerably across subjects and correlated strongly with CSF [PPX] (r = 0.97, p < 0.0001). CSF [PPX] was not related to CSF [Aβ(42)], [Tau], or [P-Tau]. Regional 18F-2DG measures of brain glucose uptake demonstrated a 3–6% decline during R(+)PPX treatment. 56 mild-moderate adverse events occurred, 26 probably/definitely related to R(+)PPX use, with 4 withdrawals. R(+)PPX was generally well-tolerated and entered brain extracellular space linearly. Further studies of R(+)PPX in AD should include a detailed pharmacokinetic study of peak and trough serum [PPX] variations among subjects prior to planning any larger studies that would be needed to determine efficacy in altering disease progression.
Keywords: Alzheimer’s disease, biomarkers, cognitive disorder, investigational treatment, oxidative stress, PET scan
DOI: 10.3233/JAD-150788
Journal: Journal of Alzheimer's Disease, vol. 49, no. 4, pp. 1179-1187, 2016
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