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Precision proteoform design for 4R tau isoform selective templated aggregation

Title: Precision proteoform design for 4R tau isoform selective templated aggregation
Authors: Longhini, Andrew P; DuBose, Austin; Lobo, Samuel; Vijayan, Vishnu; Bai, Yeran; Rivera, Erica Keane; Sala-Jarque, Julia; Nikitina, Arina; Carrettiero, Daniel C; Unger, Matthew T; Sclafani, Olivia R; Fu, Valerie; Beckett, Emily R; Vigers, Michael; Buée, Luc; Landrieu, Isabelle; Shell, Scott; Shea, Joan E; Han, Songi; Kosik, Kenneth S
Source: Proceedings of the National Academy of Sciences of the United States of America, vol 121, iss 15
Publisher Information: eScholarship, University of California
Publication Year: 2024
Collection: University of California: eScholarship
Subject Terms: 3101 Biochemistry and Cell Biology (for-2020); 31 Biological Sciences (for-2020); Dementia (rcdc); Neurodegenerative (rcdc); Alzheimer's Disease Related Dementias (ADRD) (rcdc); Infectious Diseases (rcdc); Alzheimer's Disease (rcdc); Aging (rcdc); Acquired Cognitive Impairment (rcdc); Neurosciences (rcdc); Emerging Infectious Diseases (rcdc); Frontotemporal Dementia (FTD) (rcdc); Rare Diseases (rcdc); Brain Disorders (rcdc); Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD) (rcdc); Humans (mesh); tau Proteins (mesh); Tauopathies (mesh); Protein Isoforms (mesh); Prions (mesh); Peptides (mesh); Amino Acids (mesh); tauopathies; prion-like templating; amyloidogenic core; protein misfolding
Description: Prion-like spread of disease-specific tau conformers is a hallmark of all tauopathies. A 19-residue probe peptide containing a P301L mutation and spanning the R2/R3 splice junction of tau folds and stacks into seeding-competent fibrils and induces aggregation of 4R, but not 3R tau. These tau peptide fibrils propagate aggregated intracellular tau over multiple generations, have a high β-sheet content, a colocalized lipid signal, and adopt a well-defined U-shaped fold found in 4R tauopathy brain-derived fibrils. Fully atomistic replica exchange molecular dynamics (MD) simulations were used to compute the free energy landscapes of the conformational ensemble of the peptide monomers. These identified an aggregation-prohibiting β-hairpin structure and an aggregation-competent U-fold unique to 4R tauopathy fibrils. Guided by MD simulations, we identified that the N-terminal-flanking residues to PHF6, which slightly vary between 4R and 3R isoforms, modulate seeding. Strikingly, when a single amino acid switch at position 305 replaced the serine of 4R tau with a lysine from the corresponding position in the first repeat of 3R tau, the seeding induced by the 19-residue peptide was markedly reduced. Conversely, a 4R tau mimic with three repeats, prepared by replacing those amino acids in the first repeat with those amino acids uniquely present in the second repeat, recovered aggregation when exposed to the 19-residue peptide. These peptide fibrils function as partial prions to recruit naive 4R tau-ten times the length of the peptide-and serve as a critical template for 4R tauopathy propagation. These results hint at opportunities for tau isoform-specific therapeutic interventions.
Document Type: article in journal/newspaper
File Description: application/pdf
Language: unknown
Relation: qt8q37m8cn; https://escholarship.org/uc/item/8q37m8cn; https://escholarship.org/content/qt8q37m8cn/qt8q37m8cn.pdf
DOI: 10.1073/pnas.2320456121
Availability: https://escholarship.org/uc/item/8q37m8cn; https://escholarship.org/content/qt8q37m8cn/qt8q37m8cn.pdf; https://doi.org/10.1073/pnas.2320456121
Rights: CC-BY-NC-ND
Accession Number: edsbas.A8C00BEC
Database: BASE