Examination of Longitudinal Alterations in Alzheimer’s Disease-Related Neurogenesis
in an APP/PS1 Transgenic Mouse Model, and the Effects of P33, a Putative Neuroprotective
Agent Thereon
Neurogenesis plays a crucial role in cognitive processes. During aging and in Alzheimer’s
disease (AD), altered neurogenesis and neuroinflammation are evident both in C57BL/6J,
APPSwe/PS1dE9 (Tg) mice and humans. AD pathology may slow down upon drug treatment,
for example, in a previous study of our group P33, a putative neuroprotective agent
was found to exert advantageous effects on the elevated levels of APP, Aβ, and neuroinflammation.
In the present study, we aimed to examine longitudinal alterations in neurogenesis,
neuroinflammation and AD pathology in a transgenic (Tg) mouse model, and assessed
the putative beneficial effects of long-term P33 treatment on AD-specific neurological
alterations. Hippocampal cell proliferation and differentiation were significantly
reduced between 8 and 12 months of age. Regarding neuroinflammation, significantly
elevated astrogliosis and microglial activation were observed in 6- to 7-month-old
Tg animals. The amounts of the molecules involved in the amyloidogenic pathway were
altered from 4 months of age in Tg animals. P33-treatment led to significantly increased
neurogenesis in 9-month-old animals. Our data support the hypothesis that altered
neurogenesis may be a consequence of AD pathology. Based on our findings in the transgenic
animal model, early pharmacological treatment before the manifestation of AD symptoms
might ameliorate neurological decline.