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Immune Recognition of β-Cells: Neoepitopes as Key Players in the Loss of Tolerance.

Citation
James, E. A., et al. “Immune Recognition Of Β-Cells: Neoepitopes As Key Players In The Loss Of Tolerance.”. Diabetes, pp. 1035-1042.
Center University of Washington Yale University
Multicenter
Multicenter
Author Eddie A James, Massimo Pietropaolo, Mark J Mamula
Abstract

Prior to the onset of type 1 diabetes, there is progressive loss of immune self-tolerance, evidenced by the accumulation of islet autoantibodies and emergence of autoreactive T cells. Continued autoimmune activity leads to the destruction of pancreatic β-cells and loss of insulin secretion. Studies of samples from patients with type 1 diabetes and of murine disease models have generated important insights about genetic and environmental factors that contribute to susceptibility and immune pathways that are important for pathogenesis. However, important unanswered questions remain regarding the events that surround the initial loss of tolerance and subsequent failure of regulatory mechanisms to arrest autoimmunity and preserve functional β-cells. In this Perspective, we discuss various processes that lead to the generation of neoepitopes in pancreatic β-cells, their recognition by autoreactive T cells and antibodies, and potential roles for such responses in the pathology of disease. Emerging evidence supports the relevance of neoepitopes generated through processes that are mechanistically linked with β-cell stress. Together, these observations support a paradigm in which neoepitope generation leads to the activation of pathogenic immune cells that initiate a feed-forward loop that can amplify the antigenic repertoire toward pancreatic β-cell proteins.

Year of Publication
2018
Journal
Diabetes
Volume
67
Issue
6
Number of Pages
1035-1042
Date Published
12/2018
ISSN Number
1939-327X
DOI
10.2337/dbi17-0030
Alternate Journal
Diabetes
PMID
29784651
PMCID
PMC5961411
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