Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology

Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology

Abnormal tau hyperphosphorylation and its aggregation into neurofibrillary tangles are a hallmark of tauopathies, neurodegenerative disorders that include Alzheimer's disease (AD). Active and passive Tau-immunotherapy has been proposed as a therapeutic approach to AD with mixed results. One of...

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Main Authors: A. Joly-Amado, H. Davtyan, K. Serraneau, P. Jules, A. Zitnyar, E. Pressman, K. Zagorski, T. Antonyan, A. Hovakimyan, H.J. Paek, M.N. Gordon, D.H. Cribbs, N. Petrovsky, M.G. Agadjanyan, A. Ghochikyan, D. Morgan
Format: Article
Language:English
Published: Elsevier 2020-02-01
Series:Neurobiology of Disease
Online Access:http://www.sciencedirect.com/science/article/pii/S0969996119303110
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spelling doaj-1cc3f32ce5154726bf49bf0ad1a97a382021-03-22T12:48:48ZengElsevierNeurobiology of Disease1095-953X2020-02-01134Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathologyA. Joly-Amado0H. Davtyan1K. Serraneau2P. Jules3A. Zitnyar4E. Pressman5K. Zagorski6T. Antonyan7A. Hovakimyan8H.J. Paek9M.N. Gordon10D.H. Cribbs11N. Petrovsky12M.G. Agadjanyan13A. Ghochikyan14D. Morgan15USF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USA; Corresponding author.The Institute for Molecular Medicine, Huntington Beach, CA 92647, USA; Institute for Memory Impairments and Neurological Disorders, University of California Irvine, Irvine, CA 92697, USAUSF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USAUSF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USAUSF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USAUSF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USAThe Institute for Molecular Medicine, Huntington Beach, CA 92647, USAThe Institute for Molecular Medicine, Huntington Beach, CA 92647, USAThe Institute for Molecular Medicine, Huntington Beach, CA 92647, USAMolecular Pharmacology and Physiology, College of Medicine, University of South Florida, Tampa, FL, USAUSF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USAInstitute for Memory Impairments and Neurological Disorders, University of California Irvine, Irvine, CA 92697, USAFlinders Med. Ctr., Bedford Park, Adelaide 5042, AustraliaThe Institute for Molecular Medicine, Huntington Beach, CA 92647, USAThe Institute for Molecular Medicine, Huntington Beach, CA 92647, USAUSF Health Byrd Alzheimer's Institute, Tampa, FL 33613, USAAbnormal tau hyperphosphorylation and its aggregation into neurofibrillary tangles are a hallmark of tauopathies, neurodegenerative disorders that include Alzheimer's disease (AD). Active and passive Tau-immunotherapy has been proposed as a therapeutic approach to AD with mixed results. One of the limitations of active immunotherapy may be associated with the mediocre immunogenicity of vaccines that are not inducing therapeutically potent titers of antibodies. The aim of this study was to test the efficacy of an anti-tau vaccine, AV-1980R/A composed of N terminal peptide of this molecule fused with an immunogenic MultiTEP platform and formulated in a strong adjuvant, AdvaxCpG in a Tg4510 mouse model of tauopathy. Experimental mice were immunized with AV-1980R/A and a control group of mice were injected with adjuvant only. Nontransgenic and tetracycline transactivator (tTA) transgenic littermates were included as baseline controls to contrast with the tau phenotype. Active immunization with AV-1980R/A induced very strong anti-tau humoral immune responses in both nontransgenic and transgenic mice with evidence of IgG in brains of AV-1980R/A vaccinated mice. These experimental animals displayed an improvement in short-term memory during a novel object recognition test. However, impairments in other behavioral tasks were not prevented by AV-1980R/A vaccinations. At the same time, high titers of anti-tau antibodies reduced hyperphosphorylated pSer396 tau but did not lower the level of other phosphorylated tau species in the brains of AV-1980R/A vaccinated mice. These data indicate that active immunotherapy with an N-terminal Tau epitope was only partially effective in improving cognition and reducing pathology in the stringent Tg4510 mouse model of tauopathy.http://www.sciencedirect.com/science/article/pii/S0969996119303110
collection DOAJ
language English
format Article
sources DOAJ
author A. Joly-Amado
H. Davtyan
K. Serraneau
P. Jules
A. Zitnyar
E. Pressman
K. Zagorski
T. Antonyan
A. Hovakimyan
H.J. Paek
M.N. Gordon
D.H. Cribbs
N. Petrovsky
M.G. Agadjanyan
A. Ghochikyan
D. Morgan
spellingShingle A. Joly-Amado
H. Davtyan
K. Serraneau
P. Jules
A. Zitnyar
E. Pressman
K. Zagorski
T. Antonyan
A. Hovakimyan
H.J. Paek
M.N. Gordon
D.H. Cribbs
N. Petrovsky
M.G. Agadjanyan
A. Ghochikyan
D. Morgan
Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology
Neurobiology of Disease
author_facet A. Joly-Amado
H. Davtyan
K. Serraneau
P. Jules
A. Zitnyar
E. Pressman
K. Zagorski
T. Antonyan
A. Hovakimyan
H.J. Paek
M.N. Gordon
D.H. Cribbs
N. Petrovsky
M.G. Agadjanyan
A. Ghochikyan
D. Morgan
author_sort A. Joly-Amado
title Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology
title_short Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology
title_full Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology
title_fullStr Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology
title_full_unstemmed Active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pSer396-tau pathology
title_sort active immunization with tau epitope in a mouse model of tauopathy induced strong antibody response together with improvement in short memory and pser396-tau pathology
publisher Elsevier
series Neurobiology of Disease
issn 1095-953X
publishDate 2020-02-01
description Abnormal tau hyperphosphorylation and its aggregation into neurofibrillary tangles are a hallmark of tauopathies, neurodegenerative disorders that include Alzheimer's disease (AD). Active and passive Tau-immunotherapy has been proposed as a therapeutic approach to AD with mixed results. One of the limitations of active immunotherapy may be associated with the mediocre immunogenicity of vaccines that are not inducing therapeutically potent titers of antibodies. The aim of this study was to test the efficacy of an anti-tau vaccine, AV-1980R/A composed of N terminal peptide of this molecule fused with an immunogenic MultiTEP platform and formulated in a strong adjuvant, AdvaxCpG in a Tg4510 mouse model of tauopathy. Experimental mice were immunized with AV-1980R/A and a control group of mice were injected with adjuvant only. Nontransgenic and tetracycline transactivator (tTA) transgenic littermates were included as baseline controls to contrast with the tau phenotype. Active immunization with AV-1980R/A induced very strong anti-tau humoral immune responses in both nontransgenic and transgenic mice with evidence of IgG in brains of AV-1980R/A vaccinated mice. These experimental animals displayed an improvement in short-term memory during a novel object recognition test. However, impairments in other behavioral tasks were not prevented by AV-1980R/A vaccinations. At the same time, high titers of anti-tau antibodies reduced hyperphosphorylated pSer396 tau but did not lower the level of other phosphorylated tau species in the brains of AV-1980R/A vaccinated mice. These data indicate that active immunotherapy with an N-terminal Tau epitope was only partially effective in improving cognition and reducing pathology in the stringent Tg4510 mouse model of tauopathy.
url http://www.sciencedirect.com/science/article/pii/S0969996119303110
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