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Efficacy and Safety of A Liposome-Based Vaccine against Protein Tau, Assessed in Tau.P301L Mice That Model Tauopathy
Author(s) -
Clara Theunis,
Natàlia CrespoBiel,
Valérie Gafner,
Maria Pihlgren,
Maria Pilar LópezDeber,
Pedro Reis,
David T. Hickman,
Oskar Adolfsson,
Nathalie Chuard,
Dorin Mlaki Ndao,
Peter Borghgraef,
Herman Devijver,
Fred Van Leuven,
Andrea Pfeifer,
Andreas Muhs
Publication year - 2013
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0072301
Subject(s) - tauopathy , neurodegeneration , tau protein , epitope , neuroscience , immunotherapy , alzheimer's disease , disease , amyloid (mycology) , biology , medicine , immune system , immunology , pathology , antibody
Progressive aggregation of protein Tau into oligomers and fibrils correlates with cognitive decline and synaptic dysfunction, leading to neurodegeneration in vulnerable brain regions in Alzheimer's disease. The unmet need of effective therapy for Alzheimer's disease, combined with problematic pharmacological approaches, led the field to explore immunotherapy, first against amyloid peptides and recently against protein Tau. Here we adapted the liposome-based amyloid vaccine that proved safe and efficacious, and incorporated a synthetic phosphorylated peptide to mimic the important phospho-epitope of protein Tau at residues pS396/pS404. We demonstrate that the liposome-based vaccine elicited, rapidly and robustly, specific antisera in wild-type mice and in Tau.P301L mice. Long-term vaccination proved to be safe, because it improved the clinical condition and reduced indices of tauopathy in the brain of the Tau.P301L mice, while no signs of neuro-inflammation or other adverse neurological effects were observed. The data corroborate the hypothesis that liposomes carrying phosphorylated peptides of protein Tau have considerable potential as safe and effective treatment against tauopathies, including Alzheimer's disease.

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