Synthesis and 11C-labelling of (E,E)-1-(3′,4′-dihydroxystyryl)-4-(3′-methoxy-4′-hydroxystyryl) benzene for PET imaging of amyloid deposits†
✍ Scribed by Yanming Wang; Chester A. Mathis; Guo-feng Huang; Daniel P. Holt; Manik L. Debnath; William E. Klunk
- Book ID
- 102372273
- Publisher
- John Wiley and Sons
- Year
- 2002
- Tongue
- French
- Weight
- 183 KB
- Volume
- 45
- Category
- Article
- ISSN
- 0022-2135
- DOI
- 10.1002/jlcr.585
No coin nor oath required. For personal study only.
✦ Synopsis
Abstract
Carboxylic acid derivatives of the amyloid‐binding dye Congo red do not enter the brain well and are thus unable to serve as in vivo amyloid‐imaging agents. A neutral amyloid probe, (E,E)‐1‐(3′,4′‐dihydroxystyryl)‐4‐(3′‐methoxy‐4′‐hydroxystyryl)benzene (3), devoid of any carboxylate groups has been designed and synthesized via a 12‐step reaction sequence with a total yield of 30%. The unsymmetric compound 3 has also been labelled with C‐11 via [^11^C]methyl iodide ([^11^C]CH~3~I) methylation of a symmetric 4,4′‐dimesyl protected precursor followed by deprotection. Preliminary evaluation indicated that compound 3 selectively stained plaques and neurofibrillary tangles in post‐mortem AD brain, and exhibited good binding affinity (K~i~=38±8 nM) for A__β__(1–40) fibrils in vitro. In vivo pharmacokinetic studies indicated that [^11^C]3 exhibited higher brain uptake than its carboxylic acid analogs and good clearance from normal control mouse brain. [^11^C]3 also exhibited specific in vivo binding to pancreatic amyloid deposits in the NOR‐beta transgenic mouse model. These results justify further investigation of 3 and similar derivatives as surrogate markers for in vivo quantitation of amyloid deposits. Copyright © 2002 John Wiley & Sons, Ltd.
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