Your search keyword '"Sekaly RP"' showing total 7 results

1. Accumulation of human immunodeficiency virus-specific cytotoxic T lymphocytes away from the predominant site of virus replication during primary infection.

Author

Pantaleo G, Soudeyns H, Demarest JF, Vaccarezza M, Graziosi C, Paolucci S, Daucher MB, Cohen OJ, Denis F, Biddison WE, Sekaly RP, and Fauci AS

Subjects

Antigen Presentation immunology, Antigens, Viral immunology, CD8-Positive T-Lymphocytes pathology, Humans, Lymph Nodes immunology, Lymph Nodes pathology, T-Lymphocyte Subsets pathology, Virus Replication immunology, CD8-Positive T-Lymphocytes immunology, Cell Movement immunology, HIV Infections immunology, HIV-1 physiology, Receptors, Antigen, T-Cell, alpha-beta immunology, T-Lymphocyte Subsets immunology

Abstract

Down-regulation of the initial burst of viremia during primary human immunodeficiency virus (HIV) infection is thought to be mediated predominantly by HIV-specific CD8+ cytotoxic T lymphocytes (CTL). This response is associated with major perturbations in the T cell receptor (TCR) repertoire. To investigate the failure of the cellular immune response to adequately control viral spread and replication and to prevent establishment of HIV infection, changes in the TCR repertoire and in the distribution of virus-specific CTL between blood and lymph node were analyzed in three patients with primary infection. By the combined use of clonotype-specific polymerase chain reaction and analysis of the frequency of in vivo activated HIV-specific CTL, it was shown that HIV-specific CTL clones preferentially accumulated in blood as opposed to lymph node. Accumulation of HIV-specific CTL in blood occurred prior to effective down-regulation of virus replication in both blood and lymph node. These findings should provide new insights into how HIV, and possibly other viruses, elude the immune response of the host during primary infection.

Published

1997

2. V alpha domain modulates the multiple topologies of mouse T cell receptor V beta20/staphylococcal enterotoxins A and E complexes.

Author

Bravo de Alba Y, Marche PN, Cazenave PA, Cloutier I, Sekaly RP, and Thibodeau J

Subjects

Animals, Antigen-Presenting Cells immunology, Enterotoxins metabolism, HLA-DR1 Antigen chemistry, Humans, Mice, Protein Binding, Receptors, Antigen, T-Cell, alpha-beta chemistry, Recombinant Proteins, Structure-Activity Relationship, Transfection, Enterotoxins immunology, HLA-DR1 Antigen metabolism, Lymphocyte Activation, Receptors, Antigen, T-Cell, alpha-beta metabolism, T-Lymphocytes immunology

Abstract

The superantigens staphylococcal enterotoxin A and E (SEA and SEE) both contact major histocompatibility complex (MHC) class II molecules on two sites located on the alpha and beta chains. We have investigated the role of the T cell receptor (TCR) alpha chain in the modulation of the various topologies of TCR/SEA (or SEE)/class II complexes. For this purpose, we have used three mouse V beta20 T cell lines expressing different V alpha domains and two T cell hybridomas expressing mouse V beta1 or V beta11 segments. The response of these T cells to SEA and SEE was studied in the context of presentation by wild-type human MHC class II molecules; or by mutants on MHC, in each of the two superantigen binding sites (position alpha39K and beta81H) to which the superantigens can still bind but with an altered conformation. Although V beta20 T cell lines are efficiently stimulated using SEA and SEE presented by wild-type HLA-DR1 molecules, our results show that the nature of the TCR V alpha domain can affect differently the recognition of the toxins bound to mutant class II molecules. This suggests that various functional topologies exist for both SEA and SEE/class II complexes and that the T cell response to each of these complexes can be modulated by the V alpha domain of the TCR. Interestingly, the recognition of SEA and SEE is achieved in different fashions by a given V beta20 T cell line.

Published

1997

3. Human immunodeficiency virus gp120 and derived peptides activate protein tyrosine kinase p56lck in human CD4 T lymphocytes.

Author

Hivroz C, Mazerolles F, Soula M, Fagard R, Graton S, Meloche S, Sekaly RP, and Fischer A

Subjects

Amino Acid Sequence, CD4 Antigens metabolism, CD4-Positive T-Lymphocytes microbiology, Enzyme Activation drug effects, Gene Products, env metabolism, HIV Envelope Protein gp120 chemistry, HIV Envelope Protein gp160, Humans, In Vitro Techniques, Lymphocyte Specific Protein Tyrosine Kinase p56(lck), Molecular Sequence Data, Molecular Weight, Peptides chemistry, Peptides pharmacology, Phosphoproteins metabolism, Phosphorylation, Phosphotyrosine, Protein Precursors metabolism, Signal Transduction, Substrate Specificity, Tyrosine analogs & derivatives, Tyrosine metabolism, CD4-Positive T-Lymphocytes enzymology, HIV Envelope Protein gp120 pharmacology, Protein-Tyrosine Kinases metabolism

Abstract

Human immunodeficiency virus binds to CD4 T lymphocytes by interaction between its envelope glycoprotein gp120 and the CD4 molecule. The latter is non-covalently associated with a src-related tyrosine kinase, p56lck. CD4 cross-linking increases the activity of p56lck, leading to phosphorylation of several cellular substrates. We report here that gp160/120 increases both the autophosphorylation of p56lck and its enzymatic activity (reflected by phosphorylation of an exogenous substrate) in normal T cells and the HUT78 CD4+ T cell line. This effect was detectable 5 min after activation and persisted for 40 min in normal T cells. It did not require gp120 cross-linking and was associated with phosphorylation of tyrosine residue on several proteins, as shown by phosphotyrosine Western blot analysis. The pattern of proteins phosphorylated on tyrosine residues in response to gp120 activation was distinct from that induced by anti-CD4 antibodies. p56lck activation required its association with CD4, since p56lck activity was not modified in HUT78 T cell lines expressing a truncated or mutated form of CD4 unable to associate with p56lck. Peptides mimicking residues 418 to 434 and 449 to 464 of HIV-1 Bru gp120, regions known to participate in gp120 binding to CD4, also increased p56lck activity and triggered phosphorylation of similar substrates. Taken together, these results show that gp160/120 and derived peptides can transiently increase p56lck activity without the need for CD4 cross-linking. This activation led to a specific pattern of tyrosine phosphorylation on cellular proteins that may be of significance in the biological effects of the gp120/CD4 interaction, e.g. syncytium formation and inhibition of T cell activation.

Published

1993

4. Direct involvement of CD7 (gp40) in activation of TcR gamma/delta+ T cells.

Author

Carrel S, Salvi S, Rafti F, Favrot M, Rapin C, and Sekaly RP

Subjects

Antibodies, Monoclonal immunology, Antigens, CD7, Calcium metabolism, Cell Line, Granulocyte-Macrophage Colony-Stimulating Factor biosynthesis, Humans, Receptors, Antigen, T-Cell, gamma-delta, Signal Transduction, Tetradecanoylphorbol Acetate pharmacology, Antigens, CD physiology, Antigens, Differentiation, T-Lymphocyte physiology, Lymphocyte Activation, Receptors, Antigen, T-Cell analysis, T-Lymphocytes immunology

Abstract

In this study we reported that on T cell receptor (TcR) gamma/delta+ cells from three cell lines Peer, MOLT-13 and ICRF-1, the T cell antigen CD7 (gp40) can be directly involved in the activation process. This is shown by a rapid increase in cytoplasmic free calcium after stimulation of these cells with an anti-CD7 monoclonal antibody (mAb). Activation through CD7 was further confirmed by measuring the production of interleukin 2 in ICRF-1 cells stimulated with anti-CD7 mAb. In addition induction of mRNA for tumor necrosis factor (TNF)-alpha and TNF-beta in Peer and for granulocyte-macrophage-colony-stimulating factor in MOLT-13 was observed in these anti-CD7-stimulated cells. The same anti-CD7 antibody was unable to activate TcR alpha/beta+ Jurkat cells or normal resting peripheral blood T lymphocytes. We further showed that normal resting TcR gamma/delta+ cells were likewise activated via the CD7 molecule. TcR gamma/delta+ cells obtained from a patient with acute lymphoblastic leukemia 3 months after autologous bone marrow transplantation were induced to proliferate, as measured by [3H]thymidine incorporation after stimulation with anti-CD7 mAb but not with anti-CD3 mAb. Interestingly TcR alpha/beta+ cells from the same donor tested in parallel were not stimulated by anti-CD7 but by anti-CD3 mAb. In essence these findings contribute to the idea that on TcR gamma/delta+ cell, the CD7 antigen could play an important role during T cell differentiation.

Published

1991

5. Binding of toxic shock syndrome toxin-1 to murine major histocompatibility complex class II molecules.

Author

Scholl PR, Sekaly RP, Diez A, Glimcher LH, and Geha RS

Subjects

Animals, Binding Sites, Enterotoxins pharmacology, HLA-DR Antigens metabolism, Lymphocyte Activation drug effects, Mice, Mice, Inbred Strains, Spleen metabolism, Bacterial Toxins, Enterotoxins metabolism, Histocompatibility Antigens Class II metabolism, Superantigens

Abstract

The staphylococcal exotoxin toxic shock syndrome toxin-1 (TSST-1) has potent stimulatory effects on murine and human lymphocytes. This is the consequence of TSST-1 binding to major histocompatibility complex (MHC) class II molecules and the engagement in a V beta-restricted fashion of the T cell receptor by the TSST-1-MHC class II complex. Using radioligand and functional assays we have recently shown that TSST-1 binds to all HLA-DR (n = 14), HLA-DQ (n = 2) and HLA-DP (n = 2) phenotypes tested. In this study, we have examined the ability of murine MHC class II molecules to bind TSST-1. Specific high-affinity binding of TSST-1 was detectable to unfractionated BALB-c (H-2d) and C57BL/6 (H-2b), but not to C3H (H-2k) spleen cells. The Kd of this binding estimated from Scatchard analysis was in the same nanomolar range as the Kd of binding of TSST-1 to HLA-DR. Binding of 125I-labeled TSST-1 to BALB/c-derived B cell lymphoma lines and to L cell transfectants correlated with the expression of I-A molecules, but not with the expression of I-E molecules. Furthermore, I-A+, I-E- cells but not I-A-, I-E+ cells were able to support TSST-1-induced T cell proliferation. The binding affinity of TSST-1 for I-Ak appears to be much lower than for I-Ad. L cell transfectants expressing hybrid DR alpha: I-E beta k molecules, but not those expressing I-E alpha k: DR1 beta molecules, could bind TSST-1 and efficiently support TSST-1-induced T cell proliferation. This suggests that minor differences in the highly homologous I-E alpha and DR alpha chains are critical in determining the affinity of the MHC class II molecule for TSST-1. These results demonstrate that the binding of TSST-1 to MHC class II molecules in the mouse, in contrast to humans, is strongly influenced by phenotype. Analysis of the molecular basis of these differences may help to localize staphylococcal exotoxin binding sites on MHC class II molecules.

Published

1990

6. Demonstration at the single-cell level of the existence of distinct clusters of epitopes in two predefined human Ia molecular subsets.

Author

Accolla RS, Sekaly RP, McDonald AP, Corte G, Gross N, and Carrel S

Subjects

Antibodies, Monoclonal immunology, Antigen-Antibody Reactions, B-Lymphocytes immunology, Cell Line, Humans, Epitopes, Histocompatibility Antigens Class II immunology

Abstract

The expression at the cell surface level of two previously defined human Ia antigen subsets, NG1 and NG2, was studied. Two monoclonal hybridoma antibodies, D1-12 (anti-NG1) and D4-22 (anti-NG2), labeled with distinct fluorochromes, were used as probes. The results indicate that NG1 and NG2 molecules are simultaneously expressed on the same cell, and moreover, that they are identifiable as spatially separate structures. In addition, when a series of 6 other anti-Ia monoclonal antibodies previously described were analyzed in a checkerboard test of binding inhibition at the cell surface level, they were found to closely mimic the reactivity pattern of either D1-12 or D4-22 antibody, suggesting that NG1 and NG2 Ia subsets express independent clusters of highly immunogenic epitopes.

Published

1982

7. Transcription of unrearranged T cell receptor delta genes in CD3- major histocompatibility complex-unrestricted cytotoxic cells.

Author

Biassoni R, Ferrini S, Sekaly RP, and Long EO

Subjects

Antigens, Differentiation, T-Lymphocyte, CD3 Complex, Clone Cells, Gene Rearrangement, T-Lymphocyte, Humans, RNA analysis, Receptors, Antigen, T-Cell analysis, Receptors, Antigen, T-Cell, gamma-delta, Lymphocytes metabolism, Major Histocompatibility Complex, Receptors, Antigen, T-Cell genetics, Transcription, Genetic

Abstract

Transcription of the T cell receptor (TcR) delta gene was detected in clones and in enriched populations of CD3- major histocompatibility complex-unrestricted cytotoxic cells. The transcripts were derived, at least in part, from unrearranged TcR delta genes, as shown by hybridization to a synthetic oligonucleotide probe corresponding to germ-line sequences just upstream of J delta 1. Transcripts from unrearranged TcR delta genes are similar in size to those from productively rearranged genes. The fact that the bulk of delta transcripts was derived from unrearranged genes was supported by the observation that TcR delta gene rearrangements were not detected in DNA isolated from an enriched CD3- cytotoxic cell population. Transcription of the TcR delta gene in CD3- cytotoxic cells is consistent with the notion that these cells belong to a T cell lineage.

Published

1989