Acta Neuropathologica Communications (Sep 2019)

Characterization of the human myelin oligodendrocyte glycoprotein antibody response in demyelination

  • Fiona Tea,
  • Joseph A. Lopez,
  • Sudarshini Ramanathan,
  • Vera Merheb,
  • Fiona X. Z. Lee,
  • Alicia Zou,
  • Deepti Pilli,
  • Ellis Patrick,
  • Anneke van der Walt,
  • Mastura Monif,
  • Esther M. Tantsis,
  • Eppie M. Yiu,
  • Steve Vucic,
  • Andrew P. D. Henderson,
  • Anthony Fok,
  • Clare L. Fraser,
  • Jeanette Lechner-Scott,
  • Stephen W. Reddel,
  • Simon Broadley,
  • Michael H. Barnett,
  • David A. Brown,
  • Jan D. Lunemann,
  • Russell C. Dale,
  • Fabienne Brilot,
  • the Australasian and New Zealand MOG Study Group

DOI
https://doi.org/10.1186/s40478-019-0786-3
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 22

Abstract

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Abstract Over recent years, human autoantibodies targeting myelin oligodendrocyte glycoprotein (MOG Ab) have been associated with monophasic and relapsing central nervous system demyelination involving the optic nerves, spinal cord, and brain. While the clinical relevance of MOG Ab detection is becoming increasingly clear as therapeutic and prognostic differences from multiple sclerosis are acknowledged, an in-depth characterization of human MOG Ab is required to answer key challenges in patient diagnosis, treatment, and prognosis. Herein, we investigated the epitope, binding sensitivity, and affinity of MOG Ab in a cohort of 139 and 148 MOG antibody-seropositive children and adults (n = 287 patients at baseline, 130 longitudinal samples, and 22 cerebrospinal fluid samples). MOG extracellular domain was also immobilized to determine the affinity of MOG Ab. MOG Ab response was of immunoglobulin G1 isotype, and was of peripheral rather than intrathecal origin. High affinity MOG Ab were detected in 15% paediatric and 18% adult sera. More than 75% of paediatric and adult MOG Ab targeted a dominant extracellular antigenic region around Proline42. MOG Ab titers fluctuated over the progression of disease, but affinity and reactivity to Proline42 remained stable. Adults with a relapsing course intrinsically presented with a reduced immunoreactivity to Proline42 and had a more diverse MOG Ab response, a feature that may be harnessed for predicting relapse. Higher titers of MOG Ab were observed in more severe phenotypes and during active disease, supporting the pathogenic role of MOG Ab. Loss of MOG Ab seropositivity was observed upon conformational changes to MOG, and this greatly impacted the sensitivity of the detection of relapsing disorders, largely considered as more severe. Careful consideration of the binding characteristics of autoantigens should be taken into account when detecting disease-relevant autoantibodies.

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