A Mutational Analysis of the Binding of Staphylococcal Enterotoxins B and C3 to the T Cell Receptor β Chain and Major Histocompatibility Complex Class II

Leder, Lukas; Llera, Andrea S.; Lavoie, Pascal M.; Lebedeva, Marina I.; Li, Hongmin; Sékaly, Rafick‐Pierre; Bohach, Gregory A.; Gahr, Pamala J.; Schlievert, Patrick M.; Karjalainen, Klaus; Mariuzza, Roy A.

doi:10.1084/jem.187.6.823

Cited by 143 publications

(131 citation statements)

References 36 publications

(63 reference statements)

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“…Expression of CD70 and CD27 antigens was monitored over a period of 6 days. SAG were used to provide a means of polyclonal T cell activation under conditions mimicking best T cell antigen receptor͞MHC͞peptide affinities in the presence of DC costimulation (23,24). Consistent with previously published data, we found that CD8 ϩ CTL uniformly and rapidly up-regulate CD70 molecules, with peak expression between day 2 and 4 as assessed by three-color flow cytometry analysis ( Fig.…”

Section: Resultssupporting

confidence: 77%

Immune regulatory loops determine productive interactions within human T lymphocyte–dendritic cell clusters

Stuhler

Zobywalski

Grünebach

et al. 1999

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

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Help for the induction of cytolytic T lymphocytes is mediated by dendritic cells (DC) that are conditioned by CD40 signaling. We identified tumor necrosis factor family member CD27L͞CD70, which is expressed by cytolytic T lymphocytes on interaction with DC to control CD154 (CD40L) up-regulation on CD45RA؉ helper T cells for subsequent DC stimulation. The results show that the initiation of a cytolytic immune response is determined by regulatory circuits, requiring simultaneous activation and differentiation of all cells involved in T lymphocyte-DC cluster formation.On activation in the periphery, early dendritic cells (DC) differentiate and move antigen into draining lymph nodes. During this process, DC lose their capacity to capture antigen. However, after maturation, DC up-regulate plasmamembrane class II molecules loaded with antigenic fragments, forming stable peptide͞major histocompatibility complexes (MHC) capable of stimulating T cells (1-3). In T cell-rich areas of lymph nodes, DC rapidly cluster with an abundant number of T lymphocytes to initiate or to anergize specific T cell responses (4).DC excel at processing and presenting exogenous viral, bacterial, tumor, and transplantation antigens in association with class I and class II MHC molecules to cytolytic T lymphocytes (CTL) and helper T cells (Th; ref. 5), and DC form long lasting and high avidity conjugates with T cells that are specific for the antigen presented (6, 7). Thus, the microenvironment for the primary induction of a cytolytic immune response is a multicell complex in which distinct cell types are in close proximity, enabling signaling by surface molecules and short-range lymphokines. Recent reports indicate that Th are required for cross-priming and efficient induction of specific CTL responses (8). In this respect, the DC is the entity that links and coordinates antigen-specific activation events by presenting epitopes for both Th and CTL (4,9).In spite of its importance, regulatory elements that initiate productive interactions within T lymphocyte-DC clusters are not defined well. Tumor necrosis factor family members CD27L͞CD70 and CD40L͞CD154 are rapidly inducible molecules preferentially expressed by lymphocytes. Although CD70 is expressed on activated, but not on resting, T cells, its ligand CD27 is expressed stably on virtually all CD45RA ϩ and, at lower levels, on the majority of CD45RO ϩ type T cells (10, 11). Disruption of CD27L͞CD70 signaling in mixed lymphocyte reactions as well as in phytohemagglutinin-, anti-CD2-, or anti-CD3-induced T cell stimulations results in abrogation of cytolytic or proliferative responses, thus underscoring the importance of this costimulatory pathway for T cell activation and T-T cell interactions (12). Moreover, recently CD27L͞ CD70 costimulation has been estimated as equal if not superior to CD80͞CD86 signaling in a mouse-tumor model in vivo (13). CD40L͞CD154 is expressed preferentially on activated, but not on resting, Th, and CD40 is expressed highly on professional antigen-presenting ...

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Section: Resultssupporting

confidence: 77%

Immune regulatory loops determine productive interactions within human T lymphocyte–dendritic cell clusters

Stuhler

Zobywalski

Grünebach

et al. 1999

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

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“…Thus, it appears that the high affinity MHC binding site can circumvent the requirement for stabilizing interactions between the TCR and MHC class II (19). Mutagenesis of SEC3 showed a direct correlation between the affinity of SEC3 for the TCR ␤-chain and mitogenicity (5). Recently, phage display was used to engineer SEC3 variants in the disulfide loop with increased affinities to the ␣/␤ TCR revealing that increasing affinity of the SEC3/TCR complex above that normally seen with SAG/TCR interactions resulted in increased T cell activation (8).…”

Section: Discussionmentioning

confidence: 99%

“…Andersen et al (6) have elegantly shown that the TCR ␣-chain interacts with the MHC ␤-chain to stabilize the trimeric complex involving SEB. Although, the TCR/SPE C/MHC class II model predicts that in this interaction SAG acts as a bridge without any direct interactions between TCR and MHC class II, SPE C contains a high affinity (K d ϭ ϳ 4 ϫ 10 Ϫ8 M), zinc-dependent, MHC class II binding domain (19), and small changes in MHC affinity can overcome larger increases in TCR affinity (5). Thus, it appears that the high affinity MHC binding site can circumvent the requirement for stabilizing interactions between the TCR and MHC class II (19).…”

Section: Discussionmentioning

confidence: 99%

“…Based on the cocrystal structure of SEC3 in contact with the mouse 14.3.d ␤-chain (21), the mutation of all SEC3 residues involved in contact with the ␤-chain revealed that only two of 12 residues (N23A, Q210A) completely lost detectable binding using their criteria for stimulatory capacity, while a third mutation (F176A) had barely detectable mitogenic activity (5). Most other SEC3 mutations did show more intermediate decreases in stimulatory capacity, which we did not observe for the TSST-1 mutants, although three SEC3 mutants showed similar minor decreases in mitogenic activity (5). These residues (Gly 102 , Lys 103 , and Gly 106 in SEC3) are located on the flexible disulfide loop and do not form hydrogen bonds with the 14.3.d TCR (21).…”

Section: Discussionmentioning

confidence: 99%

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Functional Analysis of the TCR Binding Domain of Toxic Shock Syndrome Toxin-1 Predicts Further Diversity in MHC Class II/Superantigen/TCR Ternary Complexes

McCormick

Tripp

Llera

et al. 2003

The Journal of Immunology

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Superantigens (SAGs) aberrantly alter immune system function through simultaneous interaction with lateral surfaces of MHC class II molecules on APCs and with particular variable regions of the TCR β-chain (Vβ). To further define the interface between the bacterial SAG toxic shock syndrome toxin-1 (TSST-1) and the TCR, we performed alanine scanning mutagenesis within the putative TCR binding region of TSST-1 along the central α helix adjacent to the N-terminal α helix and the β7-β9 loop as well as with two universally conserved SAG residues (Leu137 and Tyr144 in TSST-1). Mutants were analyzed for multiple functional activities, and various residues appeared to play minor or insignificant roles in the TCR interaction. The locations of six residues (Gly16, Trp116, Glu132, His135, Gln136, and Gln139), each individually critical for functional activity as well as direct interaction with the human TCR Vβ2.1-chain, indicate that the interface occurs in a novel region of the SAG molecule. Based on these data, a model of the MHC/TSST-1/TCR ternary complex predicts similarities seen with other characterized SAGs, although the CDR3 loop of Vβ2.1 is probably involved in direct SAG-TCR molecular interactions, possibly contributing to the TCR Vβ specificity of TSST-1.

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“…While this association made perfect biological sense based on the known central role of SAgs in the human disease, mice are not susceptible to SAgs due to an inherent lower affinity of mouse MHC class II molecules to GAS SAgs. The role of GAS SAgs can be well investigated in HLA class II transgenic mice as others and we have reported (Leder et al, 1998;Andersen et al, 1999;Welcher et al, 2002;Nooh et al, 2007). However, due to the overwhelming response to SAgs in these mice, it is difficult to use them to dissect host response to other GAS virulence factors in the disease process.…”

Section: Discussionmentioning

confidence: 99%

Systems Biology Approach to Identifying Host Interactive Pathways Modulating the Severity of Streptococcal Sepsis

Abdeltawab¹

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A Mutational Analysis of the Binding of Staphylococcal Enterotoxins B and C3 to the T Cell Receptor β Chain and Major Histocompatibility Complex Class II

Cited by 143 publications

References 36 publications

Immune regulatory loops determine productive interactions within human T lymphocyte–dendritic cell clusters

Immune regulatory loops determine productive interactions within human T lymphocyte–dendritic cell clusters

Functional Analysis of the TCR Binding Domain of Toxic Shock Syndrome Toxin-1 Predicts Further Diversity in MHC Class II/Superantigen/TCR Ternary Complexes

Systems Biology Approach to Identifying Host Interactive Pathways Modulating the Severity of Streptococcal Sepsis

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