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Fluent molecular mixing of Tau isoforms in Alzheimer’s disease neurofibrillary tangles

Aurelio J. Dregni, Pu Duan, Hong Xu, Lakshmi Changolkar, Nadia El Mammeri, Virginia M.-Y. Lee and Mei Hong ()
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Aurelio J. Dregni: Massachusetts Institute of Technology
Pu Duan: Massachusetts Institute of Technology
Hong Xu: University of Pennsylvania School of Medicine
Lakshmi Changolkar: University of Pennsylvania School of Medicine
Nadia El Mammeri: Massachusetts Institute of Technology
Virginia M.-Y. Lee: University of Pennsylvania School of Medicine
Mei Hong: Massachusetts Institute of Technology

Nature Communications, 2022, vol. 13, issue 1, 1-11

Abstract: Abstract Alzheimer’s disease (AD) is defined by intracellular neurofibrillary tangles formed by the microtubule-associated protein tau and extracellular plaques formed by the β-amyloid peptide. AD tau tangles contain a mixture of tau isoforms with either four (4R) or three (3R) microtubule-binding repeats. Here we use solid-state NMR to determine how 4R and 3R tau isoforms mix at the molecular level in AD tau aggregates. By seeding differentially isotopically labeled 4R and 3R tau monomers with AD brain-derived tau, we measured intermolecular contacts of the two isoforms. The NMR data indicate that 4R and 3R tau are well mixed in the AD-tau seeded fibrils, with a 60:40 incorporation ratio of 4R to 3R tau and a small homotypic preference. The AD-tau templated 4R tau, 3R tau, and mixed 4R and 3R tau fibrils exhibit no structural differences in the rigid β-sheet core or the mobile domains. Therefore, 4R and 3R tau are fluently recruited into the pathological fold of AD tau aggregates, which may explain the predominance of AD among neurodegenerative disorders.

Date: 2022
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DOI: 10.1038/s41467-022-30585-0

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