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Original Articles

Major Histocompatibility Complex Class II Molecules Function as a Template for the Processing of a Partially Processed Insulin Peptide into a T-cell Epitope

  1. Ying Lang,
  2. Frederique Forquet,
  3. Edwin Speck,
  4. Janice Blum and
  5. Terry L Delovitch
  1. Autoimmunity/Diabetes Group, The John P. Robarts Research Institute, and the Department of Microbiology and Immunology, University of Western Ontario London, Ontario, Canada Department of Microbiology and Immunology, Indiana University Indianapolis, Indiana
  1. Address correspondence and reprint requests to Dr. Terry L. Delovitch, Director, Autoimmunity/Diabetes Group, Sheldon H. Weinstein Scientist in Diabetes, The John P. Robarts Research Institute, London, Ontario N6G 2V4, Canada.
Diabetes 1996 Dec; 45(12): 1711-1719. https://doi.org/10.2337/diab.45.12.1711
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Abstract

Our understanding of how an autoantigen is processed and presented during the development of a major histocompatibility complex (MHC) class II-dependent and T-cell-mediated autoimmune disease, such as IDDM, is incompletely understood. We have used insulin as a model autoantigen in IDDM to address the question of whether MHC class II molecules play a role in the generation and/or preservation of an autoantigen peptide that stimulates T-cell activation. Analyses of the requirement of I-Ad class II molecules in the processing of the partially processed porcine insulin peptide A1-A14/B1-B16 demonstrate that the binding of this peptide to I-Ad is essential for it to be further processed and tailored into a T-cell epitope. Based on our observations, we propose a two-step model for insulin processing in which insulin is first processed by an enzyme(s) into an intermediate peptide that binds to class II and then class II functions as a template to guide the processing of this partially processed peptide by cathepsin D into a T-cell epitope. Our data further underscore the important realization that MHC class II-directed processing of an autoantigen (e.g., insulin) may regulate 1) the relative immunodominance of T-cell determinants in an autoantigen, 2) the self-reactivity to cryptic T-cell epitopes in autoantigens, and 3) the susceptibility to autoimmune disease.

  • Received March 21, 1996.
  • Revision received July 27, 1996.
  • Accepted July 27, 1996.
  • Copyright © 1996 by the American Diabetes Association

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December 1996, 45(12)
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Major Histocompatibility Complex Class II Molecules Function as a Template for the Processing of a Partially Processed Insulin Peptide into a T-cell Epitope
Ying Lang, Frederique Forquet, Edwin Speck, Janice Blum, Terry L Delovitch
Diabetes Dec 1996, 45 (12) 1711-1719; DOI: 10.2337/diab.45.12.1711

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Major Histocompatibility Complex Class II Molecules Function as a Template for the Processing of a Partially Processed Insulin Peptide into a T-cell Epitope
Ying Lang, Frederique Forquet, Edwin Speck, Janice Blum, Terry L Delovitch
Diabetes Dec 1996, 45 (12) 1711-1719; DOI: 10.2337/diab.45.12.1711
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