Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors

[Image: see text] Self-assembly of the microtubule-associated protein tau into neurotoxic oligomers, fibrils, and paired helical filaments, and cell-to-cell spreading of these pathological tau species are critical processes underlying the pathogenesis of Alzheimer’s disease and other tauopathies. Mo...

Descripción completa

Detalles Bibliográficos
Autores principales: Despres, Clément, Di, Jing, Cantrelle, François-Xavier, Li, Zizheng, Huvent, Isabelle, Chambraud, Béatrice, Zhao, Jing, Chen, Jianle, Chen, Shiguo, Lippens, Guy, Zhang, Fuming, Linhardt, Robert, Wang, Chunyu, Klärner, Frank-Gerrit, Schrader, Thomas, Landrieu, Isabelle, Bitan, Gal, Smet-Nocca, Caroline
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2019
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6636790/
https://www.ncbi.nlm.nih.gov/pubmed/31046227
http://dx.doi.org/10.1021/acschembio.9b00325
_version_ 1783436126524014592
author Despres, Clément
Di, Jing
Cantrelle, François-Xavier
Li, Zizheng
Huvent, Isabelle
Chambraud, Béatrice
Zhao, Jing
Chen, Jianle
Chen, Shiguo
Lippens, Guy
Zhang, Fuming
Linhardt, Robert
Wang, Chunyu
Klärner, Frank-Gerrit
Schrader, Thomas
Landrieu, Isabelle
Bitan, Gal
Smet-Nocca, Caroline
author_facet Despres, Clément
Di, Jing
Cantrelle, François-Xavier
Li, Zizheng
Huvent, Isabelle
Chambraud, Béatrice
Zhao, Jing
Chen, Jianle
Chen, Shiguo
Lippens, Guy
Zhang, Fuming
Linhardt, Robert
Wang, Chunyu
Klärner, Frank-Gerrit
Schrader, Thomas
Landrieu, Isabelle
Bitan, Gal
Smet-Nocca, Caroline
author_sort Despres, Clément
collection PubMed
description [Image: see text] Self-assembly of the microtubule-associated protein tau into neurotoxic oligomers, fibrils, and paired helical filaments, and cell-to-cell spreading of these pathological tau species are critical processes underlying the pathogenesis of Alzheimer’s disease and other tauopathies. Modulating the self-assembly process and inhibiting formation and spreading of such toxic species are promising strategies for therapy development. A challenge in investigating tau self-assembly in vitro is that, unlike most amyloidogenic proteins, tau does not aggregate in the absence of posttranslational modifications (PTM), aggregation inducers, or preformed seeds. The most common induction method is addition of polyanions, such as heparin; yet, this artificial system may not represent adequately tau self-assembly in vivo, which is driven by aberrant phosphorylation and other PTMs, potentially leading to in vitro data that do not reflect the behavior of tau and its interaction with modulators in vivo. To tackle these challenges, methods for in vitro phosphorylation of tau to produce aggregation-competent forms recently have been introduced (Despres et al. (2017) Proc. Natl. Acad. Sci. U.S.A., 114, 9080−908528784767). However, the oligomerization, seeding, and interaction with assembly modulators of the different forms of tau have not been studied to date. To address these knowledge gaps, we compared here side-by-side the self-assembly and seeding activity of heparin-induced tau with two forms of in vitro phosphorylated tau and tested how the molecular tweezer CLR01, a negatively charged compound, affected these processes. Tau was phosphorylated by incubation either with activated extracellular signal-regulated kinase 2 or with a whole rat brain extract. Seeding activity was measured using a fluorescence-resonance energy transfer-based biosensor-cell method. We also used solution-state NMR to investigate the binding sites of CLR01 on tau and how they were impacted by phosphorylation. Our systematic structure–activity relationship study demonstrates that heparin-induced tau behaves differently from in vitro phosphorylated tau. The aggregation rates of the different forms are distinct as is the intracellular localization of the induced aggregates, which resemble brain-derived tau strains suggesting that heparin-induced tau and in vitro phosphorylated tau have different conformations, properties, and activities. CLR01 inhibits aggregation and seeding of both heparin-induced and in vitro phosphorylated tau dose-dependently, although heparin induction interferes with the interaction between CLR01 and tau.
format Online
Article
Text
id pubmed-6636790
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher American Chemical Society
record_format MEDLINE/PubMed
spelling pubmed-66367902019-07-18 Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors Despres, Clément Di, Jing Cantrelle, François-Xavier Li, Zizheng Huvent, Isabelle Chambraud, Béatrice Zhao, Jing Chen, Jianle Chen, Shiguo Lippens, Guy Zhang, Fuming Linhardt, Robert Wang, Chunyu Klärner, Frank-Gerrit Schrader, Thomas Landrieu, Isabelle Bitan, Gal Smet-Nocca, Caroline ACS Chem Biol [Image: see text] Self-assembly of the microtubule-associated protein tau into neurotoxic oligomers, fibrils, and paired helical filaments, and cell-to-cell spreading of these pathological tau species are critical processes underlying the pathogenesis of Alzheimer’s disease and other tauopathies. Modulating the self-assembly process and inhibiting formation and spreading of such toxic species are promising strategies for therapy development. A challenge in investigating tau self-assembly in vitro is that, unlike most amyloidogenic proteins, tau does not aggregate in the absence of posttranslational modifications (PTM), aggregation inducers, or preformed seeds. The most common induction method is addition of polyanions, such as heparin; yet, this artificial system may not represent adequately tau self-assembly in vivo, which is driven by aberrant phosphorylation and other PTMs, potentially leading to in vitro data that do not reflect the behavior of tau and its interaction with modulators in vivo. To tackle these challenges, methods for in vitro phosphorylation of tau to produce aggregation-competent forms recently have been introduced (Despres et al. (2017) Proc. Natl. Acad. Sci. U.S.A., 114, 9080−908528784767). However, the oligomerization, seeding, and interaction with assembly modulators of the different forms of tau have not been studied to date. To address these knowledge gaps, we compared here side-by-side the self-assembly and seeding activity of heparin-induced tau with two forms of in vitro phosphorylated tau and tested how the molecular tweezer CLR01, a negatively charged compound, affected these processes. Tau was phosphorylated by incubation either with activated extracellular signal-regulated kinase 2 or with a whole rat brain extract. Seeding activity was measured using a fluorescence-resonance energy transfer-based biosensor-cell method. We also used solution-state NMR to investigate the binding sites of CLR01 on tau and how they were impacted by phosphorylation. Our systematic structure–activity relationship study demonstrates that heparin-induced tau behaves differently from in vitro phosphorylated tau. The aggregation rates of the different forms are distinct as is the intracellular localization of the induced aggregates, which resemble brain-derived tau strains suggesting that heparin-induced tau and in vitro phosphorylated tau have different conformations, properties, and activities. CLR01 inhibits aggregation and seeding of both heparin-induced and in vitro phosphorylated tau dose-dependently, although heparin induction interferes with the interaction between CLR01 and tau. American Chemical Society 2019-05-02 2019-06-21 /pmc/articles/PMC6636790/ /pubmed/31046227 http://dx.doi.org/10.1021/acschembio.9b00325 Text en Copyright © 2019 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Despres, Clément
Di, Jing
Cantrelle, François-Xavier
Li, Zizheng
Huvent, Isabelle
Chambraud, Béatrice
Zhao, Jing
Chen, Jianle
Chen, Shiguo
Lippens, Guy
Zhang, Fuming
Linhardt, Robert
Wang, Chunyu
Klärner, Frank-Gerrit
Schrader, Thomas
Landrieu, Isabelle
Bitan, Gal
Smet-Nocca, Caroline
Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors
title Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors
title_full Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors
title_fullStr Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors
title_full_unstemmed Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors
title_short Major Differences between the Self-Assembly and Seeding Behavior of Heparin-Induced and in Vitro Phosphorylated Tau and Their Modulation by Potential Inhibitors
title_sort major differences between the self-assembly and seeding behavior of heparin-induced and in vitro phosphorylated tau and their modulation by potential inhibitors
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6636790/
https://www.ncbi.nlm.nih.gov/pubmed/31046227
http://dx.doi.org/10.1021/acschembio.9b00325
work_keys_str_mv AT despresclement majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT dijing majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT cantrellefrancoisxavier majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT lizizheng majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT huventisabelle majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT chambraudbeatrice majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT zhaojing majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT chenjianle majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT chenshiguo majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT lippensguy majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT zhangfuming majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT linhardtrobert majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT wangchunyu majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT klarnerfrankgerrit majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT schraderthomas majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT landrieuisabelle majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT bitangal majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors
AT smetnoccacaroline majordifferencesbetweentheselfassemblyandseedingbehaviorofheparininducedandinvitrophosphorylatedtauandtheirmodulationbypotentialinhibitors

Ejemplares similares