Structure of an Autoimmune T Cell Receptor Complexed with Class II Peptide-MHCInsights into MHC Bias and Antigen Specificity

Maynard, Jennifer A.; Petersson, Karin; Wilson, Darcy B.; Adams, E. Eric; Blondelle, Sylvie E.; Boulanger, M; Wilson, Dianne H.; Garcia, K. Chrisopher

doi:10.1016/s1074-7613(04)00378-4

Cited by 68 publications

(144 citation statements)

References 0 publications

Supporting

Mentioning

139

Contrasting

Order By: Relevance

“…Changes in flanks or in MHC contact residues have been found to affect TCR recognition and, in some instances, the flank residue may serve as a TCR contact, although this is not always the case. Perhaps, as indicated by the three reports on the structures of T cell receptors bound to myelin basic protein peptide-MHC complexes, it points to the need for broader contacts between both the peptide-MHC and the T cell receptors (41)(42)(43).…”

Section: Discussionmentioning

confidence: 99%

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

View full text Add to dashboard Cite

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.

show abstract

Section: Discussionmentioning

confidence: 99%

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

View full text Add to dashboard Cite

show abstract

“…The crystal structure of autoreactive TCR-MHC class II complexes reveals that TCR predominantly contacts/recognizes the MHC molecule, while few contact points exist between the CDR3 loop of the TCR and the presented peptide [9]. Our approach with stimulatory APM provides a conceptual framework that enables us to address the autoreactive TCR repertoire selection.…”

Section: Discussionmentioning

confidence: 99%

Degenerate TCR recognition and dual DR2 restriction of autoreactive T cells: Implications for the initiation of the autoimmune response in multiple sclerosis

et al. 2008

View full text Add to dashboard Cite

TCR degeneracy may facilitate self-reactive T cell activation and the initiation of an autoimmune response in multiple sclerosis (MS). MHC class II alleles of the DR2 haplotype DR2a (DRB5*0101) and DR2b (DRB1*1501) are associated with an increased risk for MS in Caucasian populations. In order to selectively expand and characterize T cells with a high degree of TCR degeneracy that recognize peptides in the context of disease-associated DR2 alleles, we developed DR2-anchored peptide mixtures (APM). We report here that DR2-APM have a high stimulatory potency and can selectively expand T cells with a degenerate TCR (TCR deg ). Due to the low concentration of individual peptides in the mixtures, T cell clones' proliferative response to DR2-APM implies that multiple peptides stimulate the TCR, which is a characteristic of TCR deg . The frequency of DR2-APM-reactive T cells is significantly higher in MS patients than in healthy controls, suggesting that they may play a role in the development of the autoimmune response in MS. DR2-APM-reactive cells have a dual DR2 restriction: they recognize DR2-APM in the context of both DR2a and DR2b molecules. The DR2-APM-reactive cells' IL-17 secretion, together with cross-reactivity against myelin peptides, may contribute to their role in the development of autoimmune response in MS.

show abstract

“…The Ag-recognizing receptors on T cells (TCRs) of the adaptive immune system are αβ-heterodimers that structurally resemble the Ag-binding (Fab) fragment of Abs. Like Abs, TCRs are encoded by genes formed by gene segment rearrangements, and most T cells express a singular TCR (61)(62)(63)(64)(65)(66) A structural basis for the puzzling propensity of TCRs to "see" MHC proteins is emerging from detailed comparisons of TCR-pMHC crystal structures (70)(71)(72)(73)(74). These show that in complementarity determining regions of the TCR (CDR1 and CDR2), there are some conserved residues that interact with various conserved combinations of MHC residues in the helices that flank the epitope-binding groove.…”

Section: T-cell Specificitymentioning

confidence: 99%

Evolving concepts of specificity in immune reactions

Eisen

Chakraborty

2010

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Our goal is to provide a perspective on current understanding of the origins of specificity in immune reactions, a topic that has intrigued scientists for over a century. A fundamental property of adaptive immune responses is the ability to discriminate among an immense variety of substances by means of antibodies (Abs) and Ab-like receptors on T lymphocytes [T-cell receptors (TCRs)], each able to bind a particular chemical structure [the antigen (Ag)] and not, or only weakly, similar alternatives. Evidence has long existed, however, and has grown, especially recently, that while exhibiting remarkable specificity, many individual Abs and TCRs can also bind a variety of very different ligands. How can Ag recognition by these receptors exercise the great specificity for which they are renowned and yet react with a variety of different ligands (degeneracy)? We critically consider the mechanistic bases for this specificity/degeneracy enigma and also compare and contrast Ag recognition by Abs and TCRs.T cells | peptide-MHC complexes | receptor-ligand interactions | antibody isomerism

show abstract

Structure of an Autoimmune T Cell Receptor Complexed with Class II Peptide-MHCInsights into MHC Bias and Antigen Specificity

Cited by 68 publications

References 0 publications

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

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

Degenerate TCR recognition and dual DR2 restriction of autoreactive T cells: Implications for the initiation of the autoimmune response in multiple sclerosis

Evolving concepts of specificity in immune reactions

Contact Info

Product

Resources

About