Reduction of αSYN Pathology in a Mouse Model of PD Using a Brain-Penetrating Bispecific Antibody

Author:

Roshanbin Sahar,Julku UlrikaORCID,Xiong MengfeiORCID,Eriksson JonasORCID,Masliah Eliezer,Hultqvist GretaORCID,Bergström Joakim,Ingelsson Martin,Syvänen Stina,Sehlin DagORCID

Abstract

Immunotherapy targeting aggregated alpha-synuclein (αSYN) is a promising approach for the treatment of Parkinson’s disease. However, brain penetration of antibodies is hampered by their large size. Here, RmAbSynO2-scFv8D3, a modified bispecific antibody that targets aggregated αSYN and binds to the transferrin receptor for facilitated brain uptake, was investigated to treat αSYN pathology in transgenic mice. Ex vivo analyses of the blood and brain distribution of RmAbSynO2-scFv8D3 and the unmodified variant RmAbSynO2, as well as in vivo analyses with microdialysis and PET, confirmed fast and efficient brain uptake of the bispecific format. In addition, intravenous administration was shown to be superior to intraperitoneal injections in terms of brain uptake and distribution. Next, aged female αSYN transgenic mice (L61) were administered either RmAbSynO2-scFv8D3, RmAbSynO2, or PBS intravenously three times over five days. Levels of TBS-T soluble aggregated αSYN in the brain following treatment with RmAbSynO2-scFv8D3 were decreased in the cortex and midbrain compared to RmAbSynO2 or PBS controls. Taken together, our results indicate that facilitated brain uptake of αSYN antibodies can improve treatment of αSYN pathology.

Funder

Swedish Research Council

Swedish Innovation Agency

Hjärnfonden

Torsten Söderbergs Stiftelse

Åke Wibergs Stiftelse

Petrus och Augusta Hedlunds Stiftelse

Åhlén-Stiftelsen

Parkinsonfonden

Magnus Bergvalls Stiftelse

Stiftelsen för Gamla Tjänarinnor

Stohnes stiftelse

Demensfonden

Konung Gustaf V:s och Drottning Victorias frimurarestiftelse

Publisher

MDPI AG

Subject

Pharmaceutical Science

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