Enhancing or Suppressive Effects of Antibodies on Processing of a Pathogenic T Cell Epitope in Thyroglobulin

Author:

Dai Yang1,Carayanniotis Karen A.1,Eliades Petros2,Lymberi Peggy2,Shepherd Philip3,Kong Yi-chi M.4,Carayanniotis George1

Affiliation:

1. *Faculty of Medicine, Memorial University of Newfoundland, St. John’s, Newfoundland, Canada;

2. †Department of Immunology, Hellenic Pasteur Institute, Athens, Greece;

3. ‡Department of Immunobiology, Guy’s, King’s College, and St. Thomas’s Hospitals’ Medical and Dental Schools, London, United Kingdom; and

4. §Department of Immunology and Microbiology, Wayne State University School of Medicine, Detroit, MI 48202

Abstract

AbstractThyroglobulin (Tg)-specific Abs occur commonly in thyroid disease, but it is not clear to what extent they affect Tg processing and presentation to T cells. Here we show that generation of the nondominant pathogenic Tg epitope (2549–2560), containing thyroxine (T4) at position 2553 (T4(2553)), is augmented by Tg-specific IgG mAbs that facilitate FcR-mediated internalization of Tg. However, other mAbs of the same (IgG1) subclass enhanced Tg uptake by APC but had no effect on the generation of this peptide. Treatment of APC with chloroquine or glutaraldehyde abrogated enhanced generation of T4(2553). The boosting effect was selective, since the enhancing mAbs did not facilitate generation of the neighboring cryptic (2495–2511) peptide, which is also pathogenic in mice. When Tg was simultaneously complexed to a mAb reactive with T4(2553) and to a mixture of boosting mAbs, the presentation of this epitope was totally suppressed. These results suggest that Tg-specific Abs alter Tg processing and may boost or suppress the presentation of nondominant pathogenic determinants during the course of disease.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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