Frontiers in Immunology (Apr 2024)

Molecular dissection of an immunodominant epitope in Kv1.2-exclusive autoimmunity

  • Ivan Talucci,
  • Ivan Talucci,
  • Friederike A. Arlt,
  • Friederike A. Arlt,
  • Kai O. Kreissner,
  • Mahoor Nasouti,
  • Mahoor Nasouti,
  • Anna-Lena Wiessler,
  • Ramona Miske,
  • Swantje Mindorf,
  • Inga Dettmann,
  • Mehrnaz Moniri,
  • Markus Bayer,
  • Peter Broegger Christensen,
  • Ilya Ayzenberg,
  • Andrea Kraft,
  • Matthias Endres,
  • Matthias Endres,
  • Matthias Endres,
  • Matthias Endres,
  • Matthias Endres,
  • Lars Komorowski,
  • Carmen Villmann,
  • Kathrin Doppler,
  • Harald Prüss,
  • Harald Prüss,
  • Hans M. Maric

DOI
https://doi.org/10.3389/fimmu.2024.1329013
Journal volume & issue
Vol. 15

Abstract

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IntroductionSubgroups of autoantibodies directed against voltage-gated potassium channel (Kv) complex components have been associated with immunotherapy-responsive clinical syndromes. The high prevalence and the role of autoantibodies directly binding Kv remain, however, controversial. Our objective was to determine Kv autoantibody binding requirements and to clarify their contribution to the observed immune response.MethodsBinding epitopes were studied in sera (n = 36) and cerebrospinal fluid (CSF) (n = 12) from a patient cohort positive for Kv1.2 but negative for 32 common neurological autoantigens and controls (sera n = 18 and CSF n = 5) by phospho and deep mutational scans. Autoantibody specificity and contribution to the observed immune response were resolved on recombinant cells, cerebellum slices, and nerve fibers.Results83% of the patients (30/36) within the studied cohort shared one out of the two major binding epitopes with Kv1.2-3 reactivity. Eleven percent (4/36) of the serum samples showed no binding. Fingerprinting resolved close to identical sequence requirements for both shared epitopes. Kv autoantibody response is directed against juxtaparanodal regions in peripheral nerves and the axon initial segment in central nervous system neurons and exclusively mediated by the shared epitopes.DiscussionSystematic mapping revealed two shared autoimmune responses, with one dominant Kv1.2-3 autoantibody epitope being unexpectedly prevalent. The conservation of the molecular binding requirements among these patients indicates a uniform autoantibody repertoire with monospecific reactivity. The enhanced sensitivity of the epitope-based (10/12) compared with that of the cell-based detection (7/12) highlights its use for detection. The determined immunodominant epitope is also the primary immune response visible in tissue, suggesting a diagnostic significance and a specific value for routine screening.

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