Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation

Monika Zilkova; Anna Nolle; Branislav Kovacech; Eva Kontsekova; Petronela Weisova; Peter Filipcik; Rostislav Skrabana; Michal Prcina; Tomas Hromadka; Ondrej Cehlar; Gabriela Paulikova Rolkova; Denisa Maderova; Michal Novak; Norbert Zilka; Jeroen J.M. Hoozemans

doi:10.1186/s40478-020-00948-z

Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation

Monika Zilkova^*
, Anna Nolle
, Branislav Kovacech
, Eva Kontsekova
, Petronela Weisova
, Peter Filipcik
, Rostislav Skrabana
, Michal Prcina
, Tomas Hromadka
, Ondrej Cehlar
, Gabriela Paulikova Rolkova
, Denisa Maderova
, Michal Novak
, Norbert Zilka
, Jeroen J.M. Hoozemans

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Immunotherapies targeting pathological tau have recently emerged as a promising approach for treatment of neurodegenerative disorders. We have previously showed that the mouse antibody DC8E8 discriminates between healthy and pathological tau, reduces tau pathology in murine tauopathy models and inhibits neuronal internalization of AD tau species in vitro. Here we show, that DC8E8 and antibodies elicited against the first-in-man tau vaccine, AADvac1, which is based on the DC8E8 epitope peptide, both promote uptake of pathological tau by mouse primary microglia. IgG1 and IgG4 isotypes of AX004, the humanized versions of DC8E8, accelerate tau uptake by human primary microglia isolated from post-mortem aged and diseased brains. This promoting activity requires the presence of the Fc-domain of the antibodies. The IgG1 isotype of AX004 showed greater ability to promote tau uptake compared to the IgG4 isotype, while none of the antibody-tau complexes provoked increased pro-inflammatory activity of microglia. Our data suggest that IgG1 has better suitability for therapeutic development.

Original language	English
Article number	74
Journal	Acta neuropathologica communications
Volume	8
Issue number	1
DOIs	https://doi.org/10.1186/s40478-020-00948-z
Publication status	Published - 1 Jan 2020

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This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Human microglia
Humanized antibody
Tau immunotherapy
Tau uptake

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Humanized-tau-antibodies-promote-tau-uptake-by-human-microglia-without-any-increase-of-inflammation.pdfFinal published version, 2.33 MBLicence: CC BY

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Zilkova, M., Nolle, A., Kovacech, B., Kontsekova, E., Weisova, P., Filipcik, P., Skrabana, R., Prcina, M., Hromadka, T., Cehlar, O., Rolkova, G. P., Maderova, D., Novak, M., Zilka, N., & Hoozemans, J. J. M. (2020). Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation. Acta neuropathologica communications, 8(1), Article 74. https://doi.org/10.1186/s40478-020-00948-z

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title = "Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation",

abstract = "Immunotherapies targeting pathological tau have recently emerged as a promising approach for treatment of neurodegenerative disorders. We have previously showed that the mouse antibody DC8E8 discriminates between healthy and pathological tau, reduces tau pathology in murine tauopathy models and inhibits neuronal internalization of AD tau species in vitro. Here we show, that DC8E8 and antibodies elicited against the first-in-man tau vaccine, AADvac1, which is based on the DC8E8 epitope peptide, both promote uptake of pathological tau by mouse primary microglia. IgG1 and IgG4 isotypes of AX004, the humanized versions of DC8E8, accelerate tau uptake by human primary microglia isolated from post-mortem aged and diseased brains. This promoting activity requires the presence of the Fc-domain of the antibodies. The IgG1 isotype of AX004 showed greater ability to promote tau uptake compared to the IgG4 isotype, while none of the antibody-tau complexes provoked increased pro-inflammatory activity of microglia. Our data suggest that IgG1 has better suitability for therapeutic development.",

keywords = "Human microglia, Humanized antibody, Tau immunotherapy, Tau uptake",

author = "Monika Zilkova and Anna Nolle and Branislav Kovacech and Eva Kontsekova and Petronela Weisova and Peter Filipcik and Rostislav Skrabana and Michal Prcina and Tomas Hromadka and Ondrej Cehlar and Rolkova, \{Gabriela Paulikova\} and Denisa Maderova and Michal Novak and Norbert Zilka and Hoozemans, \{Jeroen J.M.\}",

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doi = "10.1186/s40478-020-00948-z",

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Zilkova, M, Nolle, A, Kovacech, B, Kontsekova, E, Weisova, P, Filipcik, P, Skrabana, R, Prcina, M, Hromadka, T, Cehlar, O, Rolkova, GP, Maderova, D, Novak, M, Zilka, N & Hoozemans, JJM 2020, 'Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation', Acta neuropathologica communications, vol. 8, no. 1, 74. https://doi.org/10.1186/s40478-020-00948-z

TY - JOUR

T1 - Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation

AU - Zilkova, Monika

AU - Nolle, Anna

AU - Kovacech, Branislav

AU - Kontsekova, Eva

AU - Weisova, Petronela

AU - Filipcik, Peter

AU - Skrabana, Rostislav

AU - Prcina, Michal

AU - Hromadka, Tomas

AU - Cehlar, Ondrej

AU - Rolkova, Gabriela Paulikova

AU - Maderova, Denisa

AU - Novak, Michal

AU - Zilka, Norbert

AU - Hoozemans, Jeroen J.M.

PY - 2020/1/1

Y1 - 2020/1/1

N2 - Immunotherapies targeting pathological tau have recently emerged as a promising approach for treatment of neurodegenerative disorders. We have previously showed that the mouse antibody DC8E8 discriminates between healthy and pathological tau, reduces tau pathology in murine tauopathy models and inhibits neuronal internalization of AD tau species in vitro. Here we show, that DC8E8 and antibodies elicited against the first-in-man tau vaccine, AADvac1, which is based on the DC8E8 epitope peptide, both promote uptake of pathological tau by mouse primary microglia. IgG1 and IgG4 isotypes of AX004, the humanized versions of DC8E8, accelerate tau uptake by human primary microglia isolated from post-mortem aged and diseased brains. This promoting activity requires the presence of the Fc-domain of the antibodies. The IgG1 isotype of AX004 showed greater ability to promote tau uptake compared to the IgG4 isotype, while none of the antibody-tau complexes provoked increased pro-inflammatory activity of microglia. Our data suggest that IgG1 has better suitability for therapeutic development.

AB - Immunotherapies targeting pathological tau have recently emerged as a promising approach for treatment of neurodegenerative disorders. We have previously showed that the mouse antibody DC8E8 discriminates between healthy and pathological tau, reduces tau pathology in murine tauopathy models and inhibits neuronal internalization of AD tau species in vitro. Here we show, that DC8E8 and antibodies elicited against the first-in-man tau vaccine, AADvac1, which is based on the DC8E8 epitope peptide, both promote uptake of pathological tau by mouse primary microglia. IgG1 and IgG4 isotypes of AX004, the humanized versions of DC8E8, accelerate tau uptake by human primary microglia isolated from post-mortem aged and diseased brains. This promoting activity requires the presence of the Fc-domain of the antibodies. The IgG1 isotype of AX004 showed greater ability to promote tau uptake compared to the IgG4 isotype, while none of the antibody-tau complexes provoked increased pro-inflammatory activity of microglia. Our data suggest that IgG1 has better suitability for therapeutic development.

KW - Human microglia

KW - Humanized antibody

KW - Tau immunotherapy

KW - Tau uptake

UR - https://www.scopus.com/pages/publications/85085710903

U2 - 10.1186/s40478-020-00948-z

DO - 10.1186/s40478-020-00948-z

M3 - Article

C2 - 32471486

SN - 2051-5960

VL - 8

JO - Acta neuropathologica communications

JF - Acta neuropathologica communications

IS - 1

M1 - 74

ER -

Humanized tau antibodies promote tau uptake by human microglia without any increase of inflammation

Abstract

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Keywords

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