Antigen Presentation and T Cell Development in H2-M-Deficient Mice

Fung-Leung, Wai-Ping; Surh, Charles D.; Liljedahl, Monika; Pang, Jesse Chung Sean; Leturcq, Didier; Peterson, Per A.; Webb, Susan R.; Karlsson, Lars

doi:10.1126/science.271.5253.1278

Cited by 246 publications

(204 citation statements)

References 27 publications

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“…Selective loss of class II conformational epitopes in human somatic variants (38) and mice lacking DM function (23,24,39) closely correlates with CLIP occupancy. In contrast, considerable evidence suggests DM activities are nonessential for conformational maturation of other class II allelic products, but there are also contradictory results in the literature (18 -21, 30).…”

Section: Partially Disrupted Class II Conformational Maturationmentioning

confidence: 99%

“…The class II chain specificities (36,37) and Ii chain influences affecting expression of these conformational epitopes (10,34) have been extensively discussed. Rabbit antisera specific for determinants located in the cytoplasmic tails of the ␣-and ␤-chains were generously provided by Ronald N. Germain (YFMYSKLRVQKSTWERG), bacteriophage repressor cI peptide P [12][13][14][15][16][17][18][19][20][21][22][23][24][25][26] (LEDARRLKAIYEKKK), SWM 129 -153 GAMNKALELFRKDI-AAKYKELGYQG, the truncated variant of moth cytochrome 88 -103 previously described as DASP KKANELIAYLKQATK, the Ii chain 85-101 KPVSQMRMATPLLMRPM peptides, and biotin-conjugated variants were purchased from Quality Controlled Biochemicals (Hopkinton, MA).…”

Section: Abs and Peptidesmentioning

confidence: 99%

“…The striking accumulation of A b /CLIP complexes alongside severely reduced peptide-loading capabilities strongly argues DM activity is required to mediate CLIP release and promote occupancy by diverse peptides under physiological conditions in normal APCs. As judged by the gain of reactivity toward wild-type class II molecules, mature CD4 ϩ T cells exclusively selected on A b /CLIP complexes exhibit somewhat incomplete tolerance toward natural self-peptides (22)(23)(24). Considerable evidence suggests these animals express a semidiverse TCR repertoire (25-28).…”

mentioning

confidence: 99%

“…It also seems likely that DM actions demonstrated via these complementation assays could be influenced by many additional experimental parameters, such as abnormal expression levels and functional contributions by recipient cell lines, making it difficult to assess the significance of these observations. Current thinking about the class II pathway has been strongly influenced by studies of DM mutant mice (22)(23)(24). The loss of DM function disrupts conventional Ag presentation and causes complex defects with respect to selection of mature CD4 ϩ T cells.…”

mentioning

confidence: 99%

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Relaxed DM Requirements During Class II Peptide Loading and CD4+ T Cell Maturation in BALB/c Mice

Bikoff

Wutz

Kenty

et al. 2001

The Journal of Immunology

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Current ideas about DM actions have been strongly influenced by studies of mutant strains expressing the H-2b haplotype. To evaluate DM contributions to class II activities in BALB/c mice, we generated a novel mutation at the DMa locus via embryonic stem cell technology. Unlike long-lived Ab/class II-associated invariant chain-derived peptide (CLIP) complexes, mature Ad and Ed molecules are loosely occupied by class II-associated invariant chain-derived peptide and are SDS unstable. BALB/c DM mutants weakly express BP107 conformational epitopes and toxic shock syndrome toxin-1 superantigen-binding capabilities, consistent with partial occupancy by wild-type ligands. Near normal numbers of mature CD4+ T cells fail to undergo superantigen-mediated negative selection, as judged by TCR Vβ usage. Ag presentation assays reveal consistent differences for Ad- and Ed-restricted T cells. Indeed, the mutation leads to decreased peptide capture by Ad molecules, and in striking contrast causes enhanced peptide loading by Ed molecules. Thus, DM requirements differ for class II structural variants coexpressed under physiological conditions in the intact animal.

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Section: Partially Disrupted Class II Conformational Maturationmentioning

confidence: 99%

Section: Abs and Peptidesmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Relaxed DM Requirements During Class II Peptide Loading and CD4+ T Cell Maturation in BALB/c Mice

Bikoff

Wutz

Kenty

et al. 2001

The Journal of Immunology

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“…Although crystallographic studies have not found any evidence for this possibility (58,60), studies with conformation-dependent Abs have suggested that peptide binding can affect the conformation of MHC class I (61, 62) and class II (43,44,59,(63)(64)(65) molecules and that such subtly altered conformations can affect recognition by TCRs (57,(65)(66)(67). Our observation that none of the hybrids reactive with A b EpIi Ϫ cells recognized H2-DM-deficient cells, and vice versa (Table I), is consistent with this idea.…”

Section: Peptide-dependence Of Alloreactive T Cell Responsesmentioning

confidence: 99%

The Alloreactive and Self-Restricted CD4+ T Cell Response Directed Against a Single MHC Class II/Peptide Combination

Kovalik

Singh

Mendiratta

et al. 2000

The Journal of Immunology

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The cellular basis for allograft rejection derives from the strong T cell response to cells bearing foreign MHC. While it was originally assumed that alloreactive T cells focus their recognition on the polymorphic residues that differ between syngeneic and allogeneic MHC molecules, studies with MHC class I-restricted CTL have shown that MHC-bound peptides play a critical role in allorecognition. It has been suggested that alloreactive T cells depend more strongly on interactions with the MHC molecule than with the associated peptide, but there is little evidence to support this idea. Here we have studied the alloreactive and self-restricted response directed against the class II H2-Ab molecule bound with a single peptide, Ep, derived from the H2-Eα chain. This MHC class II-peptide combination was a poor target and stimulator of alloreactive CD4+ T cell responses, indicating that MHC-bound peptides are as important for alloreactive CD4+ T cells as they are for alloreactive CTL. We also generated alloreactive T cells with exquisite specificity for the Ab/Ep complex, and compared their reactivity with self-restricted T cells specific for the same Ab/Ep complex. Our results showed that peptide-specific alloreactive T cells, as compared with self-restricted T cells, were more sensitive to peptide stimulation, but equally sensitive to amino acid substitutions in the peptide. These findings indicate that alloreactive and self-restricted T cells interact similarly with their MHC/peptide ligand.

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Peptide binding and antigen presentation by class II histocompatibility glycoproteins

Jensen

1997

Biopolymers

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The immune system has evolved complex mechanisms for the recognition and elimination of pathogens. CD4+ helper T lymphocytes play a central role in orchestrating immune responses and their activation is carefully regulated. These cells selectively recognize short peptide antigens stably associated with membrane‐bound class II histocompatibility glycoproteins that are selectively expressed in specialized antigen presenting cells. The class II—peptide complexes are generated through a series of events that occur in membrane‐bound compartments within antigen presenting cells that, collectively, have become known as the class II antigen processing pathway. In the present paper, our current understanding of this pathway is reviewed with emphasis on mechanisms that regulate peptide binding by class II histocompatibility molecules. © 1997 John Wiley & Sons, Inc. Biopoly 43: 303–322, 1997

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Antigen Presentation and T Cell Development in H2-M-Deficient Mice

Cited by 246 publications

References 27 publications

Relaxed DM Requirements During Class II Peptide Loading and CD4+ T Cell Maturation in BALB/c Mice

Relaxed DM Requirements During Class II Peptide Loading and CD4+ T Cell Maturation in BALB/c Mice

The Alloreactive and Self-Restricted CD4+ T Cell Response Directed Against a Single MHC Class II/Peptide Combination

Peptide binding and antigen presentation by class II histocompatibility glycoproteins

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