Dual role of peripheral B cells in multiple sclerosis: emerging remote players in demyelination and novel diagnostic biomarkers

Gabriel Torres Iglesias; Mireya Fernández-Fournier; MariPaz López-Molina; Dolores Piniella; Fernando Laso-García; Mari Carmen Gómez-de Frutos; Elisa Alonso-López; Lucía Botella; Beatriz Chamorro; Sara Sánchez-Velasco; Inmaculada Puertas; Antonio Tallón Barranco; Pilar Nozal; Exuperio Díez-Tejedor; María Gutiérrez-Fernández; Laura Otero-Ortega

doi:10.3389/fimmu.2023.1224217

Dual role of peripheral B cells in multiple sclerosis: emerging remote players in demyelination and novel diagnostic biomarkers

Front Immunol. 2023 Aug 10:14:1224217. doi: 10.3389/fimmu.2023.1224217. eCollection 2023.

Authors

Gabriel Torres Iglesias¹, Mireya Fernández-Fournier¹, MariPaz López-Molina¹, Dolores Piniella¹, Fernando Laso-García¹, Mari Carmen Gómez-de Frutos¹, Elisa Alonso-López¹, Lucía Botella¹, Beatriz Chamorro¹, Sara Sánchez-Velasco¹, Inmaculada Puertas¹, Antonio Tallón Barranco¹, Pilar Nozal², Exuperio Díez-Tejedor¹, María Gutiérrez-Fernández¹, Laura Otero-Ortega¹

Affiliations

¹ Neurological Sciences and Cerebrovascular Research Laboratory, Department of Neurology, Neurology and Cerebrovascular Disease Group, Neuroscience Area La Paz Hospital Institute for Health Research-IdiPAZ (La Paz University Hospital-Universidad Autónoma de Madrid), Madrid, Spain.
² Immunology Department, La Paz University Hospital, IdiPAZ Health Research Institute, Madrid, Spain.

Abstract

Introduction: Multiple sclerosis is an inflammatory and demyelinating disease caused by a pathogenic immune response against the myelin sheath surfaces of oligodendrocytes. The demyelination has been classically associated with pathogenic B cells residing in the central nervous system that release autoreactive antibodies against myelin. The aim of the present study was to investigate whether extracellular vesicles (EVs) mediate delivery of myelin autoreactive antibodies from peripheral B cells against oligodendrocytes in multiple sclerosis (MS) and to analyze whether these EVs could mediate demyelination in vitro. We also studied the role of these EV-derived myelin antibodies as a diagnostic biomarker in MS.

Methods: This is a prospective, observational, and single-center study that includes patients with MS and two control groups: patients with non-immune white matter lesions and healthy controls. We isolated B-cell-derived EVs from the blood and cerebrospinal fluid (CSF) and analyzed their myelin antibody content. We also studied whether antibody-loaded EVs reach oligodendrocytes in patients with MS and the effect on demyelination of B-cell-derived EVs containing antibodies in vitro.

Results: This study enrolled 136 MS patients, 23 white matter lesions controls, and 39 healthy controls. We found autoreactive myelin antibodies in EVs that were released by peripheral B cells, but not by populations of B cells resident in CSF. We also identified a cut-off of 3.95 ng/mL of myelin basic protein autoantibodies in EVs from peripheral B cells, with 95.2% sensitivity and 88.2% specificity, which allows us to differentiate MS patients from healthy controls. EV-derived myelin antibodies were also detected in the oligodendrocytes of MS patients. Myelin antibody-loaded EVs from B cells induced myelin markers decrease of oligodendrocytes in vitro.

Discussion: Peripheral reactive immune cells could contribute remotely to MS pathogenesis by delivering myelin antibodies to oligodendrocytes. EV-derived myelin antibodies could play a role as diagnostic biomarker in MS.

Keywords: demyelination; extracellular vesicles; multiple sclerosis; myelin antibodies; serum diagnostic biomarkers.

Copyright © 2023 Torres Iglesias, Fernández-Fournier, López-Molina, Piniella, Laso-García, Gómez-de Frutos, Alonso-López, Botella, Chamorro, Sánchez-Velasco, Puertas, Tallón Barranco, Nozal, Díez-Tejedor, Gutiérrez-Fernández and Otero-Ortega.

Publication types

Observational Study
Research Support, Non-U.S. Gov't

MeSH terms

Autoantibodies
B-Lymphocytes
Biomarkers
Central Nervous System
Humans
Multiple Sclerosis* / diagnosis

Substances

Autoantibodies
Biomarkers

Grants and funding

This work was sponsored by a grant from Miguel Servet (CP20/00024 to LO-O), Miguel Servet (CPII20/00002 to MG-F), predoctoral fellowships (FI18/00026 to FL-G, FI22/00009 to ML-M), Río-Hortega grants (CM22/00065 to GTI and CM20/00047 to EA-L) and research project PI21/000918 from the Carlos III Health Institute Health Care Research Fund and co-funded by the European Union and by a grant CA1/RSUE/2021-00753 to DP funded by Ministerio de Universidades, Plan de Recuperación, Transformación y Resiliencia y la Universidad Autónoma de Madrid.