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| Title: | Affinity-matured B cell responses neutralizing type-I interferons underlie severe viral infections | Authors: | Fournier, Morgane Vanderkerken, Matthias Dorgham, Karim Bastard, Paul Ahouzi, Olivia Duquerroy, Stephane Nguyen, Ngoc Khanh Broutin, Manon Charlet, Manon Vandenberghe, Alexis Van Endert, Paolo Bizien, Lucy Da Mata-Jardin, Omaira Ferriño-Iriarte, Andrés Haouz, Ahmed Belmondo, Thibaut Hüe, Sophie Borghesi, Alessandro Rodríguez Gallego, José Carlos Vinh, Donald C. Andreakos, Evangelos Haerynck, Filomeen Halwani, Rabih Pan-Hammarström, Qiang Björkström, Niklas K. Strunz, Benedikt Mogensen, Trine H. Piralla, Antonio Varchetta, Stefania Freixinet Gilart, Jorge Lorenzo Roussel, Lucie Trouillet Assant, Sophie Neven, Bénédicte Levy, Romain le Voyer, Tom Delmonte, Ottavia M. O’Farrelly, Cliona Rivière, Jacques Amador Borrero, Blanca Servettaz, Amélie Kouyos, Roger D. Kaufmann, Daniel E. Crickx, Etienne Michel, Marc Puel, Anne Abel, Laurent Luyt, Charles Edouard Mathian, Alexis Kisand, Kai Duffy, Darragh Quintana-Murci, Lluis Amoura, Zahir Hale, Benjamin G. Weill, Jean Claude Casanova, Jean Laurent Rey, Felix A. Gorochov, Guy Chappert, Pascal Mahévas, Matthieu |
UNESCO Clasification: | 32 Ciencias médicas 2407 Biología celular 320505 Enfermedades infecciosas |
Keywords: | Affinity Maturation Antibodies Autoimmunity B Cells Covid-19, et al |
Issue Date: | 2026 | Journal: | Cell | Abstract: | Autoantibodies neutralizing type-I interferons (AAN-I-IFNs) emerge as global, common, and strong determinants of a growing number of severe viral diseases. We report that AAN-I-IFNs+ patients with life-threatening COVID-19 pneumonia harbor circulating type-I IFN-specific B cells indistinguishable from patients bearing T cell tolerance defects of genetic origin. This autoimmune response mobilizes a highly diverse and stable circulating B cell response that is detected prior to severe viral infection and acquires high affinity and neutralization potential to type-I IFNs through extended somatic hypermutation. X-ray crystallography and AlphaFold3 structural analysis of hundreds of patient-derived monoclonal antibodies reveals the extended breadth of this response, targeting three major B cell epitopes covering all facets of type-I IFNs. These findings support a model in which a germinal-center-derived memory B cell response directed against type-I IFNs is established before severe viral infection, providing a core mechanism linking T cell tolerance defect to pathogenic AAN-I-IFNs underlying severe viral diseases. | URI: | https://accedacris.ulpgc.es/jspui/handle/10553/166323 | ISSN: | 0092-8674 | DOI: | 10.1016/j.cell.2026.04.013 | Source: | Cell [ISSN 0092-8674], (Mayo 2026) |
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