Alzheimer’s
disease (AD), a neurodegenerative disease, is
the leading cause of dementia. Sesamol is a lignan extracted from
sesame oil and has been found to exert neuroprotective effects. The
present study aimed to investigate the neuroprotective effects of
sesamol on APPswe/PS1dE9 transgenic AD mice. The AD mice were fed
with a diet supplemented with sesamol (0.075 w/w %). Sesamol treatment
improved spatial memory and learning ability in AD mice, improved
neuronal damage, and decreased Aβ accumulation. Sesamol protected
the synaptic ultrastructure and inhibited neuroinflammatory responses
in the brain of AD mice. Sesamol also significantly inhibited the
overactivated microglia and reduced the overexpression of TNF-α
and IL-1β in the brain of AD mice. Notably, sesamol reshaped
gut microbiota by significantly decreasing the relative abundance
of Helicobacter hepaticus, Clostridium, and Bacillaceae, enhancing the relative abundance
of Rikenellaceae and Bifidobacterium in AD mice.
It has been found that sesamol protected the gut barrier integrity
and prevented the LPS leakage into the serum. Importantly, sesamol
remarkably enhanced the content of SCFAs, including acetate, propionate,
isobutyrate, butyrate, and valerate, in AD mice. Correlation analysis
indicated that there was a strong correlation between the levels of
SCFAs and cognitive functions. These results demonstrated that sesamol
attenuated AD-related cognitive dysfunction and neuroinflammatory
responses, which could be partly explained by its role in mediating
the gut microbe–SCFA–brain axis. Thus, sesamol is a
promising nutritional intervention strategy to prevent AD via the
microbiota–gut–brain axis.
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