Abstract:Prion-like transmission of pathology in alpha-synucleinopathies like Parkinsons disease or multiple system atrophy is increasingly recognized as one potential mechanism to address disease progression. Active and passive immunotherapies targeting insoluble, aggregated alpha-synuclein are already being actively explored in the clinic with mixed outcomes so far. Here, we report the identification of 306C7B3, a highly selective, aggregate-specific alpha-synuclein antibody with picomolar affinity devoid of binding … Show more
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