<b>Subtype‐specific interactions of type C staphylococcal enterotoxins with the T‐cell receptor</b>

Deringer, James R.; Ely, Robert; Stauffacher, Cynthia V.; Bohach, Gregory A.

doi:10.1046/j.1365-2958.1996.1381506.x

Cited by 50 publications

(45 citation statements)

References 46 publications

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“…Only one other characterized toxin stimulates TCR V␤ 5.1 (SEE), and no other toxins have been observed to stimulate V␤ 5.2 or 6.7. The structure of the PTSAg must dictate the TCR V␤ profile of the stimulated T cells (10,16,18). It has been seen with other toxins that a large region at the top front (in the standard view of SEB and -C) or top back of TSST-1 is important for TCR binding (11,13,22,28).…”

Section: Discussionmentioning

confidence: 99%

Biochemical and Biological Properties of Staphylococcal Enterotoxin K

et al. 2001

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Staphylococcus aureus is an important human pathogen which is implicated in a wide variety of diseases. Major determinants of the virulence of this organism include extracellular virulence factors. Staphylococcal enterotoxins (SEs) are important causative agents in staphylococcal toxic shock syndrome and food poisoning. Our study identified a novel enterotoxin, SEK, and examined its biochemical and biological properties. SEK had a molecular weight of 26,000 and an experimentally determined pI of between 7.0 and 7.5. SEK was secreted by clinical isolates of S. aureus. We demonstrated that SEK had many of the biological activities associated with the SEs, including superantigenicity, pyrogenicity, the ability to enhance the lethal effect of endotoxin, and lethality in a rabbit model when administered by subcutaneous miniosmotic pump. Recombinant SEK was shown to stimulate human CD4 ؉ and CD8 ؉ T cells in a V␤-specific manner; T-cells bearing V␤ 5.1, 5.2, and 6.7 were significantly stimulated to proliferate.

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Section: Discussionmentioning

confidence: 99%

Biochemical and Biological Properties of Staphylococcal Enterotoxin K

et al. 2001

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“…An in vitro system was designed whereby human PBMC were stimulated with SEB, a superantigen with a well-characterized specificity (29), and responses were monitored among the directly activated population of V␤17 ϩ T cells and the nonspecific or bystander population of V␤13.1 ϩ T cells. There are numerous advantages to this system: a large proportion of the T cell repertoire is directly stimulated by SEB; the V␤13.1 subset is well characterized as nonresponsive to SEB (29 -32); this nonresponsive bystander subset represents a sizeable proportion of T cells in most donors, facilitating the identification of rare events; finally, and perhaps most importantly, the V region of the TCR ␤-chain is the sole determinant of superantigen specificity, and as such, the relative promiscuity of the TCR peptide recognition site is irrelevant.…”

Section: Bystander T Cells Up-regulate Early Activation Markers In Rementioning

confidence: 99%

Human CD4+ Memory T Cells Are Preferential Targets for Bystander Activation and Apoptosis

Bangs

Baban²,

Cattan³

et al. 2009

The Journal of Immunology

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There is much evidence that T cells may be activated via mechanisms that act independently of direct TCR ligation. Despite this, the question of whether such forms of bystander T cell activation occur during immune responses is hotly debated. To address some outstanding questions, we set up an in vitro system within which to analyze bystander T cell activation in human T cells, in the absence of the possibility for TCR cross-reactivity. In addition, we have investigated the genetic, phenotypic, and functional characteristics of bystander-activated T cells. In this study, we show that bystander T cell activation is, indeed, observed during a specific immune response, and that it occurs preferentially among CD4؉ memory T cells. Furthermore, bystander-activated T cells display a distinct gene expression profile. The mechanism for bystander T cell activation involves soluble factors, and the outcome is an elevated level of apoptosis. This may provide an explanation for the attrition of T cell memory pools of heterologous specificity during immune responses to pathogens such as viruses.

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“…The bacterial superantigens SEA, SEB, and SEC2 are believed to interact with one of the CDRs of the TCR (Bellio et al, 1994;Deringer, 1996;Patten et al, 1993;Pontzer et al, 1992). To determine if CDRs play a role in the SpeA-TCR interaction, we attempted to inhibit SpeA stimulation of PBMC with CDR-specific peptides.…”

Section: Spea Interacts With the Tcr Via The Cdr Regions Of The V␤ Chainmentioning

confidence: 99%

“…Two recent publications illustrate that both SEC2 and SEC3 bind the three CDR regions (Deringer et al, 1996;Fields et al 1996). Fields et al (1996) crystallized SEC3 complexed with a purified mouse V␤ chain.…”

Section: Figmentioning

confidence: 99%

“…The various superantigens appear to bind to the complementary determining regions (CDR) of the TCR V␤ chain (Bellio et al, 1994;Deringer et al, 1996;Mollick et al, 1993;Patten et al, 1993;Pontzer et al, 1992). CDR1 through CDR4 are the hypervariable, solventexposed loops formed between the ␤-sheets of the V␤ chain (Chothia et al, 1988;Davis and Bjorkman, 1988).…”

Section: Introductionmentioning

confidence: 99%

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Analysis of the interaction between the bacterial superantigen streptococcal pyrogenic exotoxin A (SpeA) and the human T‐cell receptor

1997

Molecular Microbiology

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SummaryStreptococcus pyogenes that produces the bacterial superantigen streptococcal pyrogenic exotoxin A (SpeA) is associated with outbreaks of streptococcal toxic shock syndrome (STSS) in the United States and Europe. SpeA stimulates V␤2.1, 12.2, 14.1, and 15.1-positive T cells, and the lymphokine production from the activated T cells is believed to result in the symptoms associated with STSS. The T-cell receptor (TCR)-SpeA interaction is crucial for superantigenic activity, and studies were undertaken to determine regions of both SpeA and the TCR involved in the formation of MHC/SpeA/TCR complexes. Previously, recombinant toxins encoded by speA alleles 1, 2, and 3 as well as toxins resulting from 19 distinct point mutations in speA1 were generated. Here, these 22 toxin forms were incubated with human peripheral blood mononuclear cells (PBMCs), and the percentages of T-cell blasts bearing V␤ chains 2.1, 12.2, and 14.1 were quantified by flow cytometry. The analysis indicates that the residues of SpeA needed for a productive TCR interaction differ for each V␤ chain examined. An amino acid substitution at only one site significantly affected the toxin's ability to stimulate V␤2.1-expressing T cells, three individual amino acid substitutions resulted in significant loss of ability to stimulate V␤12.2-expressing T cells, and substitution at 13 individual sites significantly affected the ability to stimulate V␤14.1-expressing T cells. To elucidate the regions of the V␤ chains that interacted with SpeA, synthetic peptides representative of the human V␤12.2 complementary-determining regions (CDRs) 1, 2, and 4 were used to block the SpeA-mediated proliferation of human PBMCs. The CDR1, CDR2 and CDR4 peptides were each able to block proliferation, with the activity of CDR1 > CDR2 > CDR4. Combinations of CDR1 peptide with CDR2 or CDR4 peptides allosterically enhanced the ability of each to block proliferation, suggesting SpeA has distinct binding sites for the CDR loops.

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Subtype‐specific interactions of type C staphylococcal enterotoxins with the T‐cell receptor

Cited by 50 publications

References 46 publications

Biochemical and Biological Properties of Staphylococcal Enterotoxin K

Biochemical and Biological Properties of Staphylococcal Enterotoxin K

Human CD4+ Memory T Cells Are Preferential Targets for Bystander Activation and Apoptosis

Analysis of the interaction between the bacterial superantigen streptococcal pyrogenic exotoxin A (SpeA) and the human T‐cell receptor

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