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• W4313343456 abstract "Abstract Mechanisms of pathogenesis of brain autoantibodies are not well defined as to functional aspects and targets in disease. We utilized V genes of Sydenham chorea derived mAb to investigate crossreactive specificities and in vivo targets after expression in Tg mice. Novel human mAb 24.3.1, derived from group A streptococcal autoimmune sequela, targeted dopamine D1 and D2 receptors and reacted with group A streptococcal carbohydrate epitope N-acetyl-beta-D-glucosamine. Anti-neuronal brain specificities included lysoganglioside on neuronal cell surface and abundant intracellular brain protein tubulin. Human mAb 24.3.1 has been shown to induce signal transduction in neuronal cells with increased Ca++ calmodulin dependent protein kinase II. Expression of chimeric IgG1a antibody in Tg mouse sera conferred reactivity with D1/D2 dopamine receptors and led to deposition on dopaminergic neurons in vivo in Tg mouse brain. IgG1a transgene was detected in vivo and in vitro with anti-allotypic antibodies against IgG1a. Immunofluorescent co-localization of allotype specific Tg antibodies and tyrosine hydroxylase demonstrated chimeric IgG1a 24.3.1 deposited and bound to dopaminergic neurons in Tg mouse brain in vivo. Tg sera and IgG1a reacted with neuronal antigens lysoganglioside, tubulin and dopamine receptors D1/D2. Our data support the hypothesis that in human disease, antibodies may bind neurons and alter brain function to induce movement and behavioral disorders such as SC and PANDAS." @default.
• W4313343456 created "2023-01-06" @default.
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• W4313343456 date "2010-04-01" @default.
• W4313343456 modified "2023-09-23" @default.
• W4313343456 title "Sydenham Chorea-derived brain autoantibody expressed in transgenic (Tg) mice targets dopaminergic neurons and reveals crossreactive anti-neuronal specificities. (93.24)" @default.
• W4313343456 doi "https://doi.org/10.4049/jimmunol.184.supp.93.24" @default.
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