Neurochondrin is a neuronal target antigen in autoimmune cerebellar degeneration

Ramona Miske; Catharina C Gross; Madeleine Scharf; Kristin S Golombeck; Marvin Hartwig; Urvashi Bhatia; Andreas Schulte-Mecklenbeck; Kathrin Bönte; Christine Strippel; Ludger Schöls; Matthis Synofzik; Hubertus Lohmann; Inga Madeleine Dettmann; Michael Deppe; Swantje Mindorf; Tobias Warnecke; Yvonne Denno; Bianca Teegen; Christian Probst; Stefanie Brakopp; Klaus-Peter Wandinger; Heinz Wiendl; Winfried Stöcker; Sven G Meuth; Lars Komorowski; Nico Melzer

doi:10.1212/NXI.0000000000000307

Neurochondrin is a neuronal target antigen in autoimmune cerebellar degeneration

Neurol Neuroimmunol Neuroinflamm. 2016 Dec 5;4(1):e307. doi: 10.1212/NXI.0000000000000307. eCollection 2017 Jan.

Authors

Ramona Miske¹, Catharina C Gross¹, Madeleine Scharf¹, Kristin S Golombeck¹, Marvin Hartwig¹, Urvashi Bhatia¹, Andreas Schulte-Mecklenbeck¹, Kathrin Bönte¹, Christine Strippel¹, Ludger Schöls¹, Matthis Synofzik¹, Hubertus Lohmann¹, Inga Madeleine Dettmann¹, Michael Deppe¹, Swantje Mindorf¹, Tobias Warnecke¹, Yvonne Denno¹, Bianca Teegen¹, Christian Probst¹, Stefanie Brakopp¹, Klaus-Peter Wandinger¹, Heinz Wiendl¹, Winfried Stöcker¹, Sven G Meuth¹, Lars Komorowski¹, Nico Melzer¹

Affiliation

¹ Institute of Experimental Immunology (R.M., M. Scharf, I.M.D., S.M., Y.D., B.T., C.P., S.B., W.S., L.K.), Euroimmun AG, Lübeck; Department of Neurology (C.C.G., K.S.G., M.H., U.B., A.S.-M., K.B., C.S., H.L., M.D., T.W., H.W., S.G.M., N.M.), University of Münster; Centre for Neurology and Hertie-Institute for Clinical Brain Research (L.S., M. Synofzik), Tübingen; German Center for Neurodegenerative Diseases (DZNE) (L.S., M. Synofzik), Tübingen; and Institute of Clinical Chemistry and Department of Neurology (K.-P.W.), University Hospital of Schleswig-Holstein, Lübeck, Germany.

Abstract

Objective: To report on a novel neuronal target antigen in 3 patients with autoimmune cerebellar degeneration.

Methods: Three patients with subacute to chronic cerebellar ataxia and controls underwent detailed clinical and neuropsychological assessment together with quantitative high-resolution structural MRI. Sera and CSF were subjected to comprehensive autoantibody screening by indirect immunofluorescence assay (IFA) and immunoblot. Immunoprecipitation with lysates of hippocampus and cerebellum combined with mass spectrometric analysis was used to identify the autoantigen, which was verified by recombinant expression in HEK293 cells and use in several immunoassays. Multiparameter flow cytometry was performed on peripheral blood and CSF, and peripheral blood was subjected to T-cell receptor spectratyping.

Results: Patients presented with a subacute to chronic cerebellar and brainstem syndrome. MRI was consistent with cortical and cerebellar gray matter atrophy associated with subsequent neuroaxonal degeneration. IFA screening revealed strong immunoglobulin G1 reactivity in sera and CSF with hippocampal and cerebellar molecular and granular layers, but not with a panel of 30 recombinantly expressed established neural autoantigens. Neurochondrin was subsequently identified as the target antigen, verified by IFA and immunoblot with HEK293 cells expressing human neurochondrin as well as the ability of recombinant neurochondrin to neutralize the autoantibodies' tissue reaction. Immune phenotyping revealed intrathecal accumulation and activation of B and T cells during the acute but not chronic phase of the disease. T-cell receptor spectratyping suggested an antigen-specific T-cell response accompanying the formation of antineurochondrin autoantibodies. No such neurochondrin reactivity was found in control cohorts of various neural autoantibody-associated neurologic syndromes, relapsing-remitting multiple sclerosis, cerebellar type of multiple system atrophy, hereditary cerebellar ataxias, other neurologic disorders, or healthy donors.

Conclusion: Neurochondrin is a neuronal target antigen in autoimmune cerebellar degeneration.