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contributor authorKuznetsov, Andrey V.
date accessioned2025-08-20T09:24:21Z
date available2025-08-20T09:24:21Z
date copyright2/26/2025 12:00:00 AM
date issued2025
identifier issn0148-0731
identifier otherbio_147_04_041003.pdf
identifier urihttp://yetl.yabesh.ir/yetl1/handle/yetl/4308223
description abstractA criterion characterizing the combined neurotoxicity of amyloid beta and tau oligomers is suggested. A mathematical model for calculating the value of this criterion during senile plaque and neurofibrillary tangle (NFT) formation is proposed. Computations show that for physiologically relevant parameter values, the value of the criterion increases approximately linearly with time. Once neurofibrillary tangles begin forming in addition to senile plaques, there is an increase in the slope characterizing the rate at which the criterion increases. The critical value of the criterion at which a neuron dies is estimated. Unless the production rates of amyloid beta and tau monomers are very large, computations predict that for the accumulated toxicity to reach the critical value, the neural machinery responsible for the degradation of amyloid beta and tau monomers and aggregates must become dysfunctional. The value of the criterion after 20 years of the aggregation process is strongly influenced by the deposition rates of amyloid beta and tau oligomers into senile plaques and NFTs. This suggests that deposition of amyloid beta and tau oligomers into senile plaques and NFTs may reduce accumulated toxicity by sequestering more toxic oligomeric species into less toxic insoluble aggregates.
publisherThe American Society of Mechanical Engineers (ASME)
titleEvaluating the Combined Neurotoxicity of Amyloid Beta and Tau Oligomers in Alzheimer's Disease: A Novel Cellular-Level Criterion
typeJournal Paper
journal volume147
journal issue4
journal titleJournal of Biomechanical Engineering
identifier doi10.1115/1.4067701
journal fristpage41003-1
journal lastpage41003-12
page12
treeJournal of Biomechanical Engineering:;2025:;volume( 147 ):;issue: 004
contenttypeFulltext


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