A pathogenetic role for the thymoma in myasthenia gravis. Autosensitization of IL-4- producing T cell clones recognizing extracellular acetylcholine receptor epitopes presented by minority class II isotypes. (original) (raw)
Research Article Free access | 10.1172/JCI2068
A M Moody, P Moss, I Roxanis, J Curnow, D Beeson, N Pantic, J Newsom-Davis, A Vincent, and N Willcox
Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Neuroscience Group, Institute for Molecular Medicine, University of Oxford, OX3 9DS, United Kingdom.
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Published May 15, 1998 -More info
Published May 15, 1998 -Version history
Myasthenia gravis (MG) is caused by helper T cell-dependent autoantibodies against the muscle acetylcholine receptor (AChR). Thymic epithelial tumors (thymomas) occur in 10% of MG patients, but their autoimmunizing potential is unclear. They express mRNAs encoding AChR alpha and epsilon subunits, and might aberrantly select or sensitize developing thymocytes or recirculating peripheral T cells against AChR epitopes. Alternatively, there could be defective self-tolerance induction in the abundant maturing thymocytes that they usually generate. For the first time, we have isolated and characterized AChR-specific T cell clones from two MG thymomas. They recognize extracellular epitopes (alpha75-90 and alpha149-158) which are processed very efficiently from muscle AChR. Both clones express CD4 and CD8alpha, and have a Th-0 cytokine profile, producing IL-4 as well as IFN-gamma. They are restricted to HLA-DP14 and DR52a; expression of these minority isotypes was strong on professional antigen-presenting cells in the donors' tumors, although it is generally weak in the periphery. The two clones' T cell receptor beta chains are different, but their alpha chain sequences are very similar. These resemblances, and the striking contrasts with T cells previously cloned from non-thymoma patients, show that thymomas generate and actively induce specific T cells rather than merely failing to tolerize them against self antigens.
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