Cytosolic antibody receptor TRIM21 is required for effective tau immunotherapy in mouse models

Aamir S. Mukadam; Lauren V. C. Miller; Annabel E. Smith; Marina Vaysburd; Siri Aastedatter Sakya; Sophie Sanford; Sophie Keeling; Benjamin J. Tuck; Panagiotis Katsinelos; Christopher Green; Lise R. Skov; Sanne S. Kaalund; Stian Foss; Keith Mayes; Kevin O’Connell; Mark Wing; Claire Knox; Jessica Banbury; Edward Avezov; James B. Rowe; Michel Goedert; Jan Terje Andersen; Leo C. James; William A. McEwan

doi:10.1126/science.abn1366

Cytosolic antibody receptor TRIM21 is required for effective tau immunotherapy in mouse models

Aamir S. Mukadam(University of Cambridge), Lauren V. C. Miller(University of Cambridge), Annabel E. Smith(University of Cambridge), Marina Vaysburd(MRC Laboratory of Molecular Biology), Siri Aastedatter Sakya(Oslo University Hospital), Sophie Sanford(University of Cambridge), Sophie Keeling(University of Cambridge), Benjamin J. Tuck(University of Cambridge), Panagiotis Katsinelos(University of Cambridge), Christopher Green(University of Cambridge), Lise R. Skov(University of Cambridge), Sanne S. Kaalund(University of Cambridge), Stian Foss(Oslo University Hospital), Keith Mayes(MRC Laboratory of Molecular Biology), Kevin O’Connell(MRC Laboratory of Molecular Biology), Mark Wing(MRC Laboratory of Molecular Biology), Claire Knox(MRC Laboratory of Molecular Biology), Jessica Banbury(MRC Laboratory of Molecular Biology), Edward Avezov(University of Cambridge), James B. Rowe(University of Cambridge), Michel Goedert(MRC Laboratory of Molecular Biology), Jan Terje Andersen(Oslo University Hospital), Leo C. James(MRC Laboratory of Molecular Biology), William A. McEwan(University of Cambridge)

Science

March 31, 2023

10.1126/science.abn1366

Cited by 79Open Access

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Abstract

Aggregates of the protein tau are proposed to drive pathogenesis in neurodegenerative diseases. Tau can be targeted by using passively transferred antibodies (Abs), but the mechanisms of Ab protection are incompletely understood. In this work, we used a variety of cell and animal model systems and showed that the cytosolic Ab receptor and E3 ligase TRIM21 (T21) could play a role in Ab protection against tau pathology. Tau-Ab complexes were internalized to the cytosol of neurons, which enabled T21 engagement and protection against seeded aggregation. Ab-mediated protection against tau pathology was lost in mice that lacked T21. Thus, the cytosolic compartment provides a site of immunotherapeutic protection, which may help in the design of Ab-based therapies in neurodegenerative disease.

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