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Microbial antigen mimics activate diabetogenic CD8 T cells in NOD mice.
Citation | “Microbial Antigen Mimics Activate Diabetogenic Cd8 T Cells In Nod Mice.”. The Journal Of Experimental Medicine, pp. 2129-46. . |
Center | Yale University |
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Author | Ningwen Tai, Jian Peng, Fuqiang Liu, Elke Gulden, Youjia Hu, Xiaojun Zhang, Li Chen, Susan Wong, Li Wen |
Abstract |
Both animal model and human studies indicate that commensal bacteria may modify type 1 diabetes (T1D) development. However, the underlying mechanisms by which gut microbes could trigger or protect from diabetes are not fully understood, especially the interaction of commensal bacteria with pathogenic CD8 T cells. In this study, using islet-specific glucose-6-phosphatase catalytic subunit-related protein (IGRP)-reactive CD8 T cell receptor NY8.3 transgenic nonobese diabetic mice, we demonstrated that MyD88 strongly modulates CD8(+) T cell-mediated T1D development via the gut microbiota. Some microbial protein peptides share significant homology with IGRP. Both the microbial peptide mimic of Fusobacteria and the bacteria directly activate IGRP-specific NY8.3 T cells and promote diabetes development. Thus, we provide evidence of molecular mimicry between microbial antigens and an islet autoantigen and a novel mechanism by which the diabetogenicity of CD8(+) T cells can be regulated by innate immunity and the gut microbiota. |
Year of Publication |
2016
|
Journal |
The Journal of experimental medicine
|
Volume |
213
|
Issue |
10
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Number of Pages |
2129-46
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Date Published |
12/2016
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ISSN Number |
1540-9538
|
DOI |
10.1084/jem.20160526
|
Alternate Journal |
J. Exp. Med.
|
PMID |
27621416
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PMCID |
PMC5030808
|
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