Find in Library

Amyloid-&#946; (A&#946;) peptides play a crucial role in the pathogenesis of Alzheimer&#8217;s disease (AD). A&#946; production, aggregation, and clearance are thought to be important therapeutic targets for AD. Curcumin has been known to have an anti-amyloidogenic effect on AD. In the present study, we performed screening analysis using a curcumin derivative library with the aim of finding derivatives effective in suppressing A&#946; production with improved bioavailability of curcumin using CHO cells that stably express human amyloid-&#946; precursor protein and using human neuroblastoma SH-SY5Y cells. We found that the curcumin derivative GT863/PE859, which has been shown to have an inhibitory effect on A&#946; and tau aggregation in vivo, was more effective than curcumin itself in reducing A&#946; secretion. We further found that GT863 inhibited neither &#946;- nor &#947;-secretase activity, but did suppress &#947;-secretase-mediated cleavage in a substrate-dependent manner. We further found that GT863 suppressed <i>N</i>-linked glycosylation, including that of the &#947;-secretase subunit nicastrin. We also found that mannosidase inhibitors that block the mannose trimming step of <i>N</i>-glycosylation suppressed A&#946; production in a similar fashion, as was observed as a result of treatment with GT863. Collectively, these results suggest that GT863 downregulates <i>N</i>-glycosylation, resulting in suppression of A&#946; production without affecting secretase activity.