Deficiency of the autoimmune regulator AIRE in thymomas is insufficient to elicit autoimmune polyendocrinopathy syndrome type 1 (APS‐1)

6533b832fe1ef96bd129a576

RESEARCH PRODUCT

Deficiency of the autoimmune regulator AIRE in thymomas is insufficient to elicit autoimmune polyendocrinopathy syndrome type 1 (APS‐1)

Philipp Ströbel M Lahti Ralf Gold Christof Burek K.v. Toyka Berthold Schalke Nick Willcox Peter Rieckmann Astrid Murumägi Hans Konrad Müller-hermelink Anthony Meager Pärt Peterson Alexander Marx Wilfried Nix Reinhild Klein R Pujoll‐borrell Kai Krohn M Luster Andreas Rosenwald

subject

Adult Male Thymoma Adolescent Thymoma Antibodies Neoplasm Thymus Gland medicine.disease_cause Autoantigens Autoimmune Diseases Pathology and Forensic Medicine Autoimmunity 03 medical and health sciences 0302 clinical medicine Antigens Neoplasm Interferon Myasthenia Gravis medicine Humans Polyendocrinopathies Autoimmune Aged Autoantibodies 030304 developmental biology Aged 80 and over 0303 health sciences biology business.industry Autoantibody Thymus Neoplasms Middle Aged Autoimmune regulator medicine.disease Immunohistochemistry Myasthenia gravis Neoplasm Proteins 3. Good health Thymic Tissue 030220 oncology & carcinogenesis Interferon Type I Immunology biology.protein Cytokines Female Antibody business Transcription Factors medicine.drug

description

Thymomas are thymic epithelial neoplasms, associated with a variety of autoimmune disorders (especially myasthenia gravis), that apparently result from aberrant intra-tumourous thymopoiesis and export of inefficiently tolerized T-cells to the periphery. The autoimmune regulator (AIRE) drives the expression of self-antigens in the thymic medulla and plays an essential role in ‘central’ tolerance in both humans and mice. However, while inactivating AIRE mutations result in the ‘autoimmune polyendocrinopathy syndrome type 1’ (APS-1), its major features are not well reproduced in AIRE-knock-out mice. Therefore, alternative human disease scenarios with concomitant AIRE deficiency may be valuable tools to test conclusions drawn from mouse models. Here we show, in a large series, that ∼95% of thymoma patients are ‘chimeric’; expression of AIRE and major AIRE-related autoantigens (eg insulin) were undetectable in their tumours but maintained in their remnant thymic tissue and lymph nodes. Notably, despite the AIRE-deficient thymopoiesis in thymomas, disorders and autoantibodies typical of APS-1 were distinctly uncommon in these patients. The one striking similarity was in the recently observed neutralizing anti-type I interferon (IFN) antibodies, which are found at diagnosis in 100% of patients with APS-1 and in ∼60% of patients with thymomas, as we show here. We conclude that APS-1 type autoantigens must be protected from autoimmunity by mechanisms that do not extend to the muscle autoantigens so frequently targeted in thymoma patients but so rarely recognized in APS-1. Thus our findings argue strongly for a tolerogenic function of AIRE beyond its role in negative T-cell selection in human thymopoiesis, and/or for specific autoimmunization against muscle in thymomas. Copyright © 2007 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

year	journal	country	edition	language
2007-03-02	The Journal of Pathology

https://doi.org/10.1002/path.2141