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Conventional DCs sample and present myelin antigens in the healthy CNS and allow parenchymal T cell entry to initiate neuroinflammation.

Sci Immunol. 2019-01; 
MundtSarah,MrdjenDunja,UtzSebastian G,GreterMelanie,SchreinerBettina,BecherBurk
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Recombinant Proteins After 9 days, splenocytes and lymph node (inguinal, axillary, and brachial) cells were cultured in complete RPMI (10% fetal calf serum, penicillin/ streptomycin, and -mercaptoethanol) containing MOG35–55 (20 g/ml; GenScript) Get A Quote

摘要

The central nervous system (CNS) is under close surveillance by immune cells, which mediate tissue homeostasis, protection, and repair. Conversely, in neuroinflammation, dysregulated leukocyte invasion into the CNS leads to immunopathology and neurological disability. To invade the brain parenchyma, autoimmune encephalitogenic T helper (T) cells must encounter their cognate antigens (Ags) presented via local Ag-presenting cells (APCs). The precise identity of the APC that samples, processes, and presents CNS-derived Ags to autoaggressive T cells is unknown. Here, we used a combination of high-dimensional single-cell mapping and conditional MHC class II ablation across all CNS APCs to systemati... More

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