(K141934) Támogató: Hungarian National Research, Development and Innovation Office
(K138763) Támogató: NKFIH
(TKP2021-EGA-16)
(Hungarian Brain Research Program 3.0 (NAP 3.0) 2022–2025)
The prevalence of Alzheimer’s disorder (AD) is increasing worldwide, and the co-morbid
anxiety is an important, albeit often neglected problem, which might appear early
during disease development. Animal models can be used to study this question. Mice,
as prey animals, show an innate defensive response against a predator odor, providing
a valuable tool for anxiety research. Our aim was to test whether the triple-transgenic
mice model of AD shows signs of innate anxiety, with specific focus on the temporal
appearance of the symptoms. We compared 3xTg-AD mice bearing human mutations of amyloid
precursor protein, presenilin 1, and tau with age-matched controls. First, separate
age-groups (between 2 and 18 months) were tested for the avoidance of 2-methyl-2-thiazoline,
a fox odor component. To test whether hypolocomotion is a general sign of innate anxiety,
open-field behavior was subsequently followed monthly in both sexes. The 3xTg-AD mice
showed more immobility, approached the fox odor container less often, and spent more
time in the avoidance zone. This effect was detectable already in two-month-old animals
irrespective of sex, not visible around six months of age, and was more pronounced
in aged females than males. The 3xTg-AD animals moved generally less. They also spent
less time in the center of the open-field, which was detectable mainly in females
older than five months. In contrast to controls, the aged 3xTg-AD was not able to
habituate to the arena during a 30-min observation period irrespective of their sex.
Amyloid beta and phospho-Tau accumulated gradually in the hippocampus, amygdala, olfactory
bulb, and piriform cortex. In conclusion, the early appearance of predator odor- and
open space-induced innate anxiety detected already in two-month-old 3xTg-AD mice make
this genetically predisposed strain a good model for testing anxiety both before the
onset of AD-related symptoms as well as during the later phase. Synaptic dysfunction
by protein deposits might contribute to these disturbances.
