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A single T cell epitope drives the neutralizing anti-drug antibody response to natalizumab in multiple sclerosis patients.

Nat Med. 2019; 
Cassotta Antonino,Mikol Vincent,Bertrand Thomas,Pouzieux Stéphanie,Le Parc Josiane,Ferrari Paul,Dumas Jacques,Auer Michael,Deisenhammer Florian,Gastaldi Matteo,Franciotta Diego,Silacci-Fregni Chiara,Fernandez Rodriguez Blanca,Giacchetto-Sasselli Isabella,Foglierini Mathilde,Jarrossay David,Geiger Roger,Sallusto Federica,Lanzavecchia Antonio,Piccoli
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Mammalian Expression System Briefly, synthetic genes expressing the NZM heavy chain and light chain variable regions (KEGG DRUG Database entry: D06886) were produced by Genscript and subcloned into vectors for expression of chimeric human CH1-murine IgG2a heavy chain (mFc) and human Igκ, respectively. Get A Quote

摘要

Natalizumab (NZM), a humanized monoclonal IgG4 antibody to α4 integrins, is used to treat patients with relapsing-remitting multiple sclerosis (MS), but in about 6% of the cases persistent neutralizing anti-drug antibodies (ADAs) are induced leading to therapy discontinuation. To understand the basis of the ADA response and the mechanism of ADA-mediated neutralization, we performed an in-depth analysis of the B and T cell responses in two patients. By characterizing a large panel of NZM-specific monoclonal antibodies, we found that, in both patients, the response was polyclonal and targeted different epitopes of the NZM idiotype. The neutralizing activity was acquired through somatic mutations an... More

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