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Toxin-Coupled MHC Class I Tetramers Can Specifically Ablate Autoreactive CD8+ T Cells and Delay Diabetes in Nonobese Diabetic Mice.

J Immunol.. 2010-04;  184(8):4196 - 4204
Benjamin G. Vincent, Ellen F. Young, Adam S. Buntzman, Rosemary Stevens, Thomas B. Kepler, Roland M. Tisch, Jeffrey A. Frelinger, and Paul R. Hess. Department of Microbiology and Immunology, University of North Carolina, Chapel Hill, NC 27599, USA.
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摘要

There is compelling evidence that self-reactive CD8(+) T cells are a major factor in development and progression of type 1 diabetes in animals and humans. Hence, great effort has been expended to define the specificity of autoimmune CD8(+) T cells and to alter their responses. Much work has focused on tolerization of T cells using proteins or peptides. A weakness in this approach is that residual autoreactive T cells may be activated and exacerbate disease. In this report, we use a novel approach, toxin-coupled MHC class I tetramers. Used for some time to identify Ag-specific cells, in this study, we use that same property to delete the Ag-specific cells. We show that saporin-coupled tetramers can delete islet-... More

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