4.6 Article

Precocious White Matter Inflammation and Behavioural Inflexibility Precede Learning and Memory Impairment in the TgAPP21 Rat Model of Alzheimer Disease

Journal

MOLECULAR NEUROBIOLOGY
Volume 58, Issue 10, Pages 5014-5030

Publisher

SPRINGER
DOI: 10.1007/s12035-021-02476-w

Keywords

Ageing; Alzheimer disease; Behavioral flexibility; Executive function; Microglia; White matter

Categories

Funding

  1. Natural Sciences and Engineering Research Council of Canada [435819, 418489]
  2. Canadian Consortium on Neurodegeneration in Aging, the Canadian Institutes of Health Research [126127]
  3. Canadian Foundation for Innovation [34213]

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The study found that behavioral inflexibility and white matter inflammation in AD accelerate compared to normal aging, and may precede impairments in learning and memory.
Neuroinflammation and behavioural inflexibility are both common in late adulthood but far more profound in Alzheimer disease (AD). To investigate the relationship between ageing, AD, neuroinflammation, and behavioural flexibility, male wild-type Fischer 344 (Wt) and the transgenic APP21 (TgAPP21) rats were aged to 4, 8, 13, and 22 months and evaluated for neuroinflammation and cognitive impairment. TgAPP21 rats overexpress a pathogenic variant of the human amyloid precursor protein (hAPP; Swedish and Indiana mutations) but do not spontaneously develop overt pathology related to AD. In both genotypes, learning and memory were similarly impaired in older rats. However, at 8 months of age, TgAPP21 rats demonstrated behavioural inflexibility in set shifting, reversal, and the Morris water maze, while Wt rats showed inflexibility at 13 and 22 months of age. This early inflexibility in TgAPP21 rats was accompanied by a precocious increase in microglia activation within the corpus callosum; 8- and 13-month-old TgAPP21 rats had similar levels of microglia activation as 13- and 22-month-old Wt rats, respectively. However, while neuroinflammation within the white matter continued to progress with age, behavioural inflexibility peaked in 8-month-old TgAPP21 rats; in older TgAPP21 rats, memory and learning impairments masked inflexibility. These findings suggest that the behavioural inflexibility and white matter inflammation seen in normal ageing are accelerated in AD and may precede impairments of learning and memory.

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