An autoantigenic T cell epitope forms unstable complexes with class II MHC: a novel route for escape from tolerance induction

Fairchild, Paul J.; Wildgoose, Richard; Atherton, Eric; Webb, Simon J.; Wraith, David C.

doi:10.1093/intimm/5.9.1151

Cited by 180 publications

(139 citation statements)

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“…The extent and specificity of these self peptide-MHC complexes in facilitating activation of antigen-specific T cells needs to be examined in greater detail. As a side note, earlier work in the experimental autoimmune encephalomyelitis model had also suggested a relationship between low affinity peptides and T cell autoreactivity [46,47]. In this inducible disease model, the autoantigenic peptide, Ac1-11 of myelin basic protein, bound poorly to the class II MHC molecule, I-A u , and autoreactive T cells were shown to escape negative selection in the thymus [46,47].…”

Section: Weak Mhc Binding Peptides and Autoreactivity: The Case Of Thmentioning

confidence: 76%

Do the peptide-binding properties of diabetogenic class II molecules explain autoreactivity?

Suri

Levisetti

Unanue

2008

Current Opinion in Immunology

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One seminal aspect in autoimmune diabetes is antigen presentation of beta cell antigens by the diabetes-propensity class II histocompatibility molecules. The binding properties of I-A g7 molecules are reviewed here and an emphasis is placed on their selection of peptides with a highly specific sequence motif, in which one or more acidic amino acids are found at the carboxy end interacting at the P9 anchoring site of I-A g7 . The reasons for the central role of I-A g7 in the autoimmune response are analyzed. The insulin B chain segment 9-23 is a hot spot for T cell selection and a striking example of a weak MHC binding peptide that triggers autoreactivity.

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Section: Weak Mhc Binding Peptides and Autoreactivity: The Case Of Thmentioning

confidence: 76%

Do the peptide-binding properties of diabetogenic class II molecules explain autoreactivity?

Suri

Levisetti

Unanue

2008

Current Opinion in Immunology

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“…In the case of the diabetic NOD mouse, previous studies (36,37) identified a high number of autoreactive T cells. These were attributed to the I-A g7 molecule, indicating that this MHC molecule in general had a propensity for high autoreactivity.…”

Section: Discussionmentioning

confidence: 96%

The Insulin-Specific T Cells of Nonobese Diabetic Mice Recognize a Weak MHC-Binding Segment in More Than One Form

Levisetti

Suri

Petzold

et al. 2007

The Journal of Immunology

108

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Several naturally occurring anti-insulin CD4 T cells were isolated from islet infiltrates of NOD mice. In accordance with the results of others, these T cells recognized the segment of the β-chain from residues 9–23. Peptides encompassing the B:(9–23) sequence bound weakly to I-Ag7 in two main contiguous registers in which two residues at the carboxyl end, P20Gly and P21Glu, influenced binding and T cell reactivity. Naturally occurring insulin-reactive T cells exhibited differing reactivities with the carboxyl-terminal amino acids, although various single residue changes in either the flanks or the core segments affected T cell responses. The insulin peptides represent another example of a weak MHC-binding ligand that is highly immunogenic, giving rise to distinct populations of autoimmune T cells.

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“…The PI-1(47-64) epitope represents a striking example of a very poor binding MHC ligand, IC 50 values ϳ100 mol/l, that gives rise to T-cells capable of causing diabetes in adoptive transfer experiments. The relationship between poor peptide-MHC binding and the fostering of an autoimmune, pathogenic T-cell repertoire has been suggested in studies on experimental allergic encephalomyelitis (7,8) and in our recent work on the insulin ␤-chain (9 -23) epitope (2) and in other model systems (9 -11).…”

Section: Discussionmentioning

confidence: 99%

“…The relationship of low affinity of a peptide to an MHC molecule and autoimmune reactivity has also been noted in the encephalitogenic peptide from myelin basic protein (7,8). This has led to the speculation that low-affinity peptides may not be conducive to the normal mechanisms in the thymus that control autoreactivity.…”

mentioning

confidence: 99%

Weak Proinsulin Peptide–Major Histocompatibility Complexes Are Targeted in Autoimmune Diabetes in Mice

et al. 2008

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OBJECTIVE— Weak major histocompatibility complex (MHC) binding of self-peptides has been proposed as a mechanism that may contribute to autoimmunity by allowing for escape of autoreactive T-cells from the thymus. We examined the relationship between the MHC-binding characteristics of a β-cell antigen epitope and T-cell autoreactivity in a model of autoimmune diabetes. RESEARCH DESIGN AND METHODS— The binding of a proinsulin epitope, proinsulin-1(47–64) (PI-1[47–64]), to the MHC class II molecules I-A g7 and I-A k was measured using purified class II molecules. T-cell reactivity to the proinsulin epitope was examined in I-A g7+ and I-A k+ mice. RESULTS— C-peptide epitopes bound very weakly to I-A g7 molecules. However, C-peptide–reactive T-cells were induced after immunization in I-A g7 –bearing mice (NOD and B6.g7) but not in I-A k –bearing mice (B10.BR and NOD. h 4). T-cells reactive with the PI-1(47–64) peptide were found spontaneously in the peripancreatic lymph nodes of pre-diabetic NOD mice. These T-cells were activated by freshly isolated β-cells in the presence of antigen-presenting cells and caused diabetes when transferred into NOD.scid mice. CONCLUSIONS— These data demonstrate an inverse relationship between self-peptide–MHC binding and T-cell autoreactivity for the PI-1(47–64) epitope in autoimmune diabetes.

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An autoantigenic T cell epitope forms unstable complexes with class II MHC: a novel route for escape from tolerance induction

Cited by 180 publications

References 0 publications

Do the peptide-binding properties of diabetogenic class II molecules explain autoreactivity?

Do the peptide-binding properties of diabetogenic class II molecules explain autoreactivity?

The Insulin-Specific T Cells of Nonobese Diabetic Mice Recognize a Weak MHC-Binding Segment in More Than One Form

Weak Proinsulin Peptide–Major Histocompatibility Complexes Are Targeted in Autoimmune Diabetes in Mice

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