Different Patterns of Autoantibody Secretion by Peripheral Blood Mononuclear Cells in Autoimmune Nodopathies

Overview

Journal Neurol Neuroimmunol Neuroinflamm

Specialty Neurology

Date 2024 Aug 22

PMID 39173087

Authors

Sophia Rohrbacher

Sabine Seefried

Beate Hartmannsberger

Rosa Annabelle

Luise Appeltshauser

Friederike A Arlt

Dirk Bramer

Christian Dresel

Johannes Dorst

Zeynep Elmas

Christiana Franke

Christian Geis

Tobias Hogen

Sabine Krause

Martin Marziniak

Mathias Maurer

Harald Pruss

Florian Schoeberl

Bertold Schrank

Claudia Steen

Helena Teichtinger

Andrea Thieme

Lena Wessely

Alma Zernecke

Claudia Sommer

Kathrin Doppler

Affiliations

Soon will be listed here.

Abstract

Background And Objectives: Autoimmune nodopathies with antibodies against the paranodal proteins show a distinct phenotype of a severe sensorimotor neuropathy. In some patients, complete remission can be achieved after treatment with rituximab whereas others show a chronic course. For optimal planning of treatment, predicting the course of disease and therapeutic response is crucial.

Methods: We stimulated peripheral blood mononuclear cells in vitro to find out whether secretion of specific autoantibodies may be a predictor of the course of disease and response to rituximab.

Results: Three patterns could be identified: In most patients with anti-Neurofascin-155-, anti-Contactin-1-, and anti-Caspr1-IgG4 autoantibodies, in vitro production of autoantibodies was detected, indicating autoantigen-specific memory B cells and short-lived plasma cells/plasmablasts as the major source of autoantibodies. These patients generally showed a good response to rituximab. In a subgroup of patients with anti-Neurofascin-155-IgG4 autoantibodies and insufficient response to rituximab, no in vitro autoantibody production was found despite high serum titers, indicating autoantibody secretion by long-lived plasma cells outside the peripheral blood. In the patients with anti-pan-Neurofascin autoantibodies-all with a monophasic course of disease-no in vitro autoantibody production could be measured, suggesting a lack of autoantigen-specific memory B cells. In some of them, autoantibody production by unstimulated cells was detectable, presumably corresponding to high amounts of autoantigen-specific plasmablasts-well in line with a severe but monophasic course of disease.

Discussion: Our data suggest that different B-cell responses may occur in autoimmune nodopathies and may serve as markers of courses of disease and response to rituximab.

Citing Articles

Different Patterns of Autoantibody Secretion by Peripheral Blood Mononuclear Cells in Autoimmune Nodopathies.

Neurol Neuroimmunol Neuroinflamm. 2024; 11(6):e200330.

PMID: 39298720 PMC: 11413992. DOI: 10.1212/NXI.0000000000200330.

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