| Literature DB >> 33219152 |
Anne-Katrin Pröbstel1,2, Xiaoyuan Zhou3, Ryan Baumann3, Sven Wischnewski4, Michael Kutza4, Olga L Rojas5, Katrin Sellrie6, Antje Bischof3, Kicheol Kim3, Akshaya Ramesh3, Ravi Dandekar3, Ariele L Greenfield3, Ryan D Schubert3, Jordan E Bisanz7,8, Stephanie Vistnes9, Khashayar Khaleghi5, James Landefeld3, Gina Kirkish3, Friederike Liesche-Starnecker10, Valeria Ramaglia4, Sneha Singh3, Edwina B Tran3, Patrick Barba3, Kelsey Zorn3, Johanna Oechtering2, Karin Forsberg11, Lawrence R Shiow9,12, Roland G Henry3, Jennifer Graves3, Bruce A C Cree3, Stephen L Hauser3, Jens Kuhle2, Jeffrey M Gelfand3, Peter M Andersen11, Jürgen Schlegel10, Peter J Turnbaugh7,8, Peter H Seeberger6, Jennifer L Gommerman5, Michael R Wilson3, Lucas Schirmer4,13, Sergio E Baranzini1,14,15.
Abstract
Changes in gut microbiota composition and a diverse role of B cells have recently been implicated in multiple sclerosis (MS), a central nervous system (CNS) autoimmune disease. Immunoglobulin A (IgA) is a key regulator at the mucosal interface. However, whether gut microbiota shape IgA responses and what role IgA+ cells have in neuroinflammation are unknown. Here, we identify IgA-bound taxa in MS and show that IgA-producing cells specific for MS-associated taxa traffic to the inflamed CNS, resulting in a strong, compartmentalized IgA enrichment in active MS and other neuroinflammatory diseases. Unlike previously characterized polyreactive anti-commensal IgA responses, CNS IgA cross-reacts with surface structures on specific bacterial strains but not with brain tissue. These findings establish gut microbiota-specific IgA+ cells as a systemic mediator in MS and suggest a critical role of mucosal B cells during active neuroinflammation with broad implications for IgA as an informative biomarker and IgA-producing cells as an immune subset to harness for therapeutic interventions.Entities:
Year: 2020 PMID: 33219152 PMCID: PMC8043673 DOI: 10.1126/sciimmunol.abc7191
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468