Abstract
Background: Considering the heterogeneity of pathological changes occurring
in Alzheimer’s disease (AD), a therapeutic approach aimed both to neuroprotection and to
neuroinflammation reduction may prove effective. Palmitoylethanolamide (PEA) has attracted
attention for its anti-inflammatory/neuroprotective properties observed in AD animal
models.
Objective and Methods: We evaluated the protective role of PEA against
amyloid-β42 (Aβ42) toxicity on cell viability and glutamatergic
transmission in primary cultures of cerebral cortex neurons and astrocytes from the
triple-transgenic murine model of AD (3xTg-AD) and their wild-type littermates (non-Tg)
mice.
Results: Aβ42 (0.5 μM; 24 h) affects the cell viability in
cultured cortical neurons and astrocytes from non-Tg mice, but not in those from 3xTg-AD
mice. These effects were counteracted by the pretreatment with PEA (0.1 μM). Basal
glutamate levels in cultured neurons and astrocytes from 3xTg-AD mice were lower than
those observed in cultured cells from non-Tg mice. Aβ42-exposure reduced and
increased glutamate levels in non-Tg mouse cortical neurons and astrocytes, respectively.
These effects were counteracted by the pretreatment with PEA. By itself, PEA did not
affect cell viability and glutamate levels in cultured cortical neurons and astrocytes
from non-Tg or 3xTg-AD mice.
Conclusion: The exposure to Aβ42 induced toxic effects on
cultured cortical neurons and astrocytes from non-Tg mice, but not in those from 3xTg-AD
mice. Furthermore, PEA exerts differential effects against Aβ42-induced
toxicity in primary cultures of cortical neurons and astrocytes from non-Tg and 3xTg-AD
mice. In particular, PEA displays protective properties in non-Tg but not in 3xTg-AD mouse
neuronal cultured cells overexpressing Aβ.
