Histochemical visualization and diffusion MRI at 7 Tesla in the TgCRND8 transgenic model of Alzheimer’s disease |
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| Authors: | Jonathan D Thiessen Kathryn A C Glazner Solmaz Nafez Angela E Schellenberg Richard Buist Melanie Martin Benedict C Albensi |
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| Institution: | (1) Division of Neurodegenerative Disorders, St. Boniface Research Centre, Winnipeg, MB, R2H 2A6, Canada;(2) Department of Physics and Astronomy, University of Manitoba, Winnipeg, MB, R3T 2N2, Canada;(3) Department of Physics, University of Winnipeg, Winnipeg, MB, R3B 2E9, Canada;(4) Department of Pharmacology and Therapeutics, University of Manitoba, Winnipeg, MB, R3E 0W3, Canada;(5) Department of Radiology, University of Manitoba, Winnipeg, MB, R3E 0T6, Canada; |
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| Abstract: | Alzheimer’s disease (AD) is a progressive neurodegenerative disorder that has been characterized by gross cortical atrophy,
cellular neurodegeneration, reactive gliosis, and the presence of microscopic extracellular amyloid plaques and intracellular
neurofibrillary tangles. Earlier diagnoses of AD would be in the best interest of managing the patient and would allow for
earlier therapeutic intervention. By measuring the apparent diffusion coefficient (ADC) using diffusion-weighted imaging (DWI),
a type of magnetic resonance imaging (MRI), one can quantify alterations in water diffusivity resulting from microscopic structural
changes in the cell at early stages that are associated with pathophysiological processes of brain injury and/or disease progression.
Whether or not this methodology is useful for AD is a question under examination. For example, DWI in suspected AD patients
has shown increases in mean ADC values in the hippocampus and diminished diffusion anisotropy in the posterior white matter.
However, in some cases, hippocampal ADC values appear not to change in AD patients. Moreover, to our knowledge, all DWI studies
in suspected AD patients to date are technically incomplete in experimental design, because corresponding histological sections
demonstrating actual plaque deposition are lacking and so it is not clear that ADC changes actually correspond to plaque deposition.
In our study, we used DWI in the TgCRND8 transgenic model of Alzheimer’s disease in conjunction with histological techniques
and found robust plaque deposition in the transgenic strain in older animals (12–16 months old). However, we did not find
statistically significant changes (p > 0.05) in ADC values (although ADC values in TgCRND8 mice did decrease in all regions examined) in mice 12–16 months old.
Collectively, recent results from human studies and in rodent AD transgenic models support our findings and suggest that amyloid
beta plaque load is not likely the major or primary component contributing to diffusional changes, if they occur. |
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