A randomized controlled study to evaluate the effect of bexarotene on amyloid‐β and apolipoprotein E metabolism in healthy subjects

Wiley - Tập 2 Số 2 - Trang 110-120 - 2016
Kaushik Kaushik1, Michael Michael1, Philip B. Philip B.2, Tim Tim2, Joel B. Joel B.2, Randall J. Randall J.3, David M. David M.3, Gary E. Gary E.4
1ReXceptor LLC Cleveland OH USA
2C<sub>2</sub>N Diagnostics LLC St. Louis MO USA
3Department of Neurology Washington University School of Medicine, Hope Center for Neurological Disorders, Knight Alzheimer's Disease Research Center St. Louis MO USA
4Department of Neurosciences School of Medicine, Case Western Reserve University Cleveland OH USA

Tóm tắt

AbstractIntroduction

We conducted a phase Ib proof of mechanism trial to determine whether bexarotene (Targretin) increases central nervous system (CNS) apolipoprotein E (apoE) levels and alters Aβ metabolism in normal healthy individuals with the APOE ε3/ε3 genotype.

Methods

We used stable isotope labeling kinetics (SILK‐ApoE and SILK‐Aβ) to measure the effect of bexarotene on the turnover rate of apoE and Aβ peptides and stable isotope spike absolute quantitation (SISAQ) to quantitate their concentrations in the cerebrospinal fluid (CSF). Normal subjects were treated for 3 days with bexarotene (n = 3 women, 3 men, average 32 years old) or placebo (n = 6 women, average 30.2 years old) before administration of C13‐leucine and collection of plasma and CSF over the next 48 hours. Bexarotene concentrations in plasma and CSF were also measured.

Results

Oral administration of bexarotene resulted in plasma levels of 1 to 2 μM; however, only low nM levels were found in CSF. Bexarotene increased CSF apoE by 25% but had no effect on metabolism of Aβ peptides.

Discussion

Bexarotene has poor CNS penetration in normal human subjects. Drug treatment resulted in a modest increase in CSF apoE levels. The absence of an effect on Aβ metabolism is likely reflective of the low CNS levels of bexarotene achieved. This study documents the utility of SILK‐ApoE technology in measuring apoE kinetics in humans.

Trial Registration

This trial is registered at clinicaltrials.gov (NCT02061878).


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Wiley

Tập 2 Số 2

110-120

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