Frontiers in Immunology (Aug 2017)

Autoantibody Repertoire in APECED Patients Targets Two Distinct Subgroups of Proteins

  • Dmytro Fishman,
  • Dmytro Fishman,
  • Kai Kisand,
  • Christina Hertel,
  • Mike Rothe,
  • Anu Remm,
  • Maire Pihlap,
  • Priit Adler,
  • Priit Adler,
  • Jaak Vilo,
  • Jaak Vilo,
  • Aleksandr Peet,
  • Antonella Meloni,
  • Antonella Meloni,
  • Katarina Trebusak Podkrajsek,
  • Tadej Battelino,
  • Øyvind Bruserud,
  • Anette S. B. Wolff,
  • Eystein S. Husebye,
  • Nicolas Kluger,
  • Kai Krohn,
  • Annamari Ranki,
  • Hedi Peterson,
  • Hedi Peterson,
  • Adrian Hayday,
  • Pärt Peterson

DOI
https://doi.org/10.3389/fimmu.2017.00976
Journal volume & issue
Vol. 8

Abstract

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High titer autoantibodies produced by B lymphocytes are clinically important features of many common autoimmune diseases. APECED patients with deficient autoimmune regulator (AIRE) gene collectively display a broad repertoire of high titer autoantibodies, including some which are pathognomonic for major autoimmune diseases. AIRE deficiency severely reduces thymic expression of gene-products ordinarily restricted to discrete peripheral tissues, and developing T cells reactive to those gene-products are not inactivated during their development. However, the extent of the autoantibody repertoire in APECED and its relation to thymic expression of self-antigens are unclear. We here undertook a broad protein array approach to assess autoantibody repertoire in APECED patients. Our results show that in addition to shared autoantigen reactivities, APECED patients display high inter-individual variation in their autoantigen profiles, which collectively are enriched in evolutionarily conserved, cytosolic and nuclear phosphoproteins. The APECED autoantigens have two major origins; proteins expressed in thymic medullary epithelial cells and proteins expressed in lymphoid cells. These findings support the hypothesis that specific protein properties strongly contribute to the etiology of B cell autoimmunity.

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