Mechanisms of Neonatal Tolerance Induced in an Animal Model for Primary Sjögren's Syndrome by Intravenous Administration of Autoantigen

Sjogren syndrome (SS) is one of the most common autoimmune diseases. Early clinical manifestations of SS are primarily decreased tear and saliva secretion, leading to dry eye and dry mouth syndromes, but in its later stages, it can become systemic, even resulting in B cell lymphomas. The use of new animal models, coupled with new technologies, is providing exciting insights into the pathogenesis, genetic predisposition, and, possibly, early diagnosis of SS. This article reviews newly described features of SS identified in experimental animal models and their relationship to human disease. New technologies, such as genomics and proteomics, may permit identification of potential candidate genes and biomarkers for disease diagnosis. Current studies using appropriate animal models in parallel with studies of human subjects is rapidly establishing a foundation for new intervention strategies that go beyond merely treating symptoms.

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Unraveling the Pathophysiology of Sjogren Syndrome-Associated Dry Eye Disease

Nguyen

Peck

2009

The Ocular Surface

107

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Antibodies against alpha-fodrin in Sjögren's syndrome

Ulbricht

Schmidt

Witte

2003

Autoimmunity Reviews

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Cathepsin S inhibitor prevents autoantigen presentation and autoimmunity

Saegusa¹,

Ishimaru²,

Yanagi³

et al. 2002

J. Clin. Invest.

128

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The cysteine endoprotease cathepsin S mediates degradation of the MHC class II invariant chain Ii in human and mouse antigen-presenting cells. Studies described here examine the functional significance of cathepsin S inhibition on autoantigen presentation and organ-specific autoimmune diseases in a murine model for Sjögren syndrome. Specific inhibitor of cathepsin S (Clik60) in vitro markedly impaired presentation of an organ-specific autoantigen, 120-kDa α-fodrin, by interfering with MHC class II-peptide binding. Autoantigen-specific T cell responses were significantly and dose-dependently inhibited by incubation with Clik60, but not with inhibitor s of cathepsin B or L. Clik60 treatment of mouse salivary gland cells selectively inhibited autopeptide-bound class II molecules. Moreover, the treatment with Clik60 in vivo profoundly blocked lymphocytic infiltration into the salivary and lacrimal glands, abrogated a rise in serum autoantibody production, and led to recovery from autoimmune manifestations. Thus, inhibition of cathepsin S in vivo alters autoantigen presentation and development of organ-specific autoimmunity. These data identify selective inhibition of cysteine protease cathepsin S as a potential therapeutic strategy for autoimmune disease processes.

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Mechanisms of Neonatal Tolerance Induced in an Animal Model for Primary Sjögren's Syndrome by Intravenous Administration of Autoantigen

Cited by 8 publications

References 39 publications

Unraveling the Pathophysiology of Sjogren Syndrome-Associated Dry Eye Disease

Unraveling the Pathophysiology of Sjogren Syndrome-Associated Dry Eye Disease

Antibodies against alpha-fodrin in Sjögren's syndrome

Cathepsin S inhibitor prevents autoantigen presentation and autoimmunity

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