A Spontaneous Model of Experimental Autoimmune Encephalomyelitis Provides Evidence of MOG-Specific B Cell Recruitment and Clonal Expansion.

Anneli Peters,Martin Figeac,Florent Salvador,Julie Boucher,Laure Deramoudt,Nathalie Journiac,Hélène Zéphir,Frédéric Leprêtre,Lennart T Mars,Mathilde Bas,Thomas Guerrier

doi:10.3389/fimmu.2022.755900

Abstract

The key role of B cells in the pathophysiology of multiple sclerosis (MS) is supported by the presence of oligoclonal bands in the cerebrospinal fluid, by the association of meningeal ectopic B cell follicles with demyelination, axonal loss and reduction of astrocytes, as well as by the high efficacy of B lymphocyte depletion in controlling inflammatory parameters of MS. Here, we use a spontaneous model of experimental autoimmune encephalomyelitis (EAE) to study the clonality of the B cell response targeting myelin oligodendrocyte glycoprotein (MOG). In particular, 94% of SJL/j mice expressing an I-As: MOG92-106 specific transgenic T cell receptor (TCR1640) spontaneously develop a chronic paralytic EAE between the age of 60-500 days. The immune response is triggered by the microbiota in the gut-associated lymphoid tissue, while there is evidence that the maturation of the autoimmune demyelinating response might occur in the cervical lymph nodes owing to local brain drainage. Using MOG-protein-tetramers we tracked the autoantigen-specific B cells and localized their enrichment to the cervical lymph nodes and among the brain immune infiltrate. MOG-specific IgG1 antibodies were detected in the serum of diseased TCR1640 mice and proved pathogenic upon adoptive transfer into disease-prone recipients. The ontogeny of the MOG-specific humoral response preceded disease onset coherent with their contribution to EAE initiation. This humoral response was, however, not sufficient for disease induction as MOG-antibodies could be detected at the age of 69 days in a model with an average age of onset of 197 days. To assess the MOG-specific B cell repertoire we FACS-sorted MOG-tetramer binding cells and clonally expand them in vitro to sequence the paratopes of the IgG heavy chain and kappa light chains. Despite the fragility of clonally expanding MOG-tetramer binding effector B cells, our results indicate the selection of a common CDR-3 clonotype among the Igk light chains derived from both disease-free and diseased TCR1640 mice. Our study demonstrates the pre-clinical mobilization of the MOG-specific B cell response within the brain-draining cervical lymph nodes, and reiterates that MOG antibodies are a poor biomarker of disease onset and progression.

Highlights

B cells are essential components of the immune infiltrate that characterizes active demyelinating lesions in multiple sclerosis (MS)
Heterozygous TCR1640 SJL/j [36], homozygous IgHMOG C57BL/6 mice [39], and heterozygous C57BL/6 2D2 mice [40] were housed under specific pathogen-free (SPF) conditions at the animal facility of the University of Lille which is accredited by the French Ministry of Agriculture to perform experiments on live mice in appliance to the French and European regulations on care and protection of the Laboratory Animals (EC Directive 2010/63)
Significantly increased the cumulative EAE score relative to the non-transgenic littermates (NTL)-serum and PBS injected groups (Figure 3B). Both the cumulative disease score and maximum disease score increased significantly after transfer of sera from diseased TCR1640 mice (Figures 3C, D). These findings demonstrate that sera containing MOG-specific antibodies of adult TCR1640 mice exacerbate disease in EAE-prone recipients only when derived from diseased TCR1640 donor mice

Summary

Introduction

B cells are essential components of the immune infiltrate that characterizes active demyelinating lesions in multiple sclerosis (MS). The clinical relevance of antibodies is further underlined by the diagnostic value of oligoclonal bands (OCBs) that are present in the cerebrospinal fluid (CSF) of 90% of MS patients. Evidence of somatic hypermutation indicates that this is an antigen-driven process [3, 4], which occurs in the braindraining cervical lymph nodes and possibly in the meningeal ectopic lymphoid structures [5, 6]. The specificity of this adaptive immune response is composite and evolves over time [7,8,9]

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