Your search keyword '"W E Biddison"' showing total 17 results

1. Analysis of the T-cell receptor repertoire of human T-cell leukemia virus type 1 (HTLV-1) Tax-specific CD8+ cytotoxic T lymphocytes from patients with HTLV-1-associated disease: evidence for oligoclonal expansion

Author

Steven Jacobson, D Banks, W E Biddison, and U Utz

Subjects

Male, Receptors, Antigen, T-Cell, alpha-beta, T cell, Molecular Sequence Data, Immunology, Microbiology, Epitope, Cell Line, Epitopes, Antigen, immune system diseases, hemic and lymphatic diseases, Virology, HLA-A2 Antigen, Tropical spastic paraparesis, medicine, Humans, Cytotoxic T cell, Amino Acid Sequence, Cells, Cultured, DNA Primers, Human T-lymphotropic virus 1, Base Sequence, biology, T-cell receptor, virus diseases, Gene Products, tax, Middle Aged, medicine.disease, biology.organism_classification, Paraparesis, Tropical Spastic, Clone Cells, medicine.anatomical_structure, Insect Science, CD8, T-Lymphocytes, Cytotoxic, Research Article

Abstract

Human T-cell leukemia virus type 1 (HTLV-1)-associated myelopathy/tropical spastic paraparesis (HAM/TSP) is a chronic, progressive neurological disease characterized by marked degeneration of the spinal cord and the presence of antibodies against HTLV-1. Patients with HAM/TSP, but not asymptomatic carriers, show very high precursor frequencies of HTLV-1-specific CD8+ T cells in peripheral blood and cerebrospinal fluid, suggestive of a role of these T cells in the pathogenesis of the disease. In HLA-A2+ HAM/TSP patients, HTLV-1-specific T cells were demonstrated to be directed predominantly against one HTLV-1 epitope, namely, Tax11-19. In the present study, we analyzed HLA-A2-restricted HTLV-1 Tax11-19-specific cytotoxic T cells from three patients with HAM/TSP. An analysis of the T-cell receptor (TCR) repertoire of these cells revealed an absence of restricted variable (V) region usage. Different combinations of TCR V alpha and V beta genes were utilized between, but also within, the individual patients for the recognition of Tax11-19. Sequence analysis of the TCR showed evidence for an oligoclonal expansion of few founder T cells in each patient. Apparent structural motifs were identified for the CDR3 regions of the TCR beta chains. One T-cell clone could be detected within the same patient over a period of 3 years. We suggest that these in vivo clonally expanded T cells might play a role in the pathogenesis of HAM/TSP and provide information on HTLV-1-specific TCR which may elucidate the nature of the T cells that infiltrate the central nervous system in HAM/TSP patients.

Published

1996

2. Peptide recognition by two HLA-A2/Tax11-19-specific T cell clones in relationship to their MHC/peptide/TCR crystal structures

Author

S, Hausmann, W E, Biddison, K J, Smith, Y H, Ding, D N, Garboczi, U, Utz, D C, Wiley, and K W, Wucherpfennig

Subjects

Cytotoxicity, Immunologic, Protein Conformation, Molecular Sequence Data, Receptors, Antigen, T-Cell, Epitopes, T-Lymphocyte, Gene Products, tax, Lymphocyte Activation, Clone Cells, Structure-Activity Relationship, Amino Acid Substitution, HLA-A2 Antigen, Humans, Amino Acid Sequence, Crystallization, Oligopeptides, T-Lymphocytes, Cytotoxic

Abstract

The crystal structures of two human TCRs specific for a HTLV-I Tax peptide bound to HLA-A2 were recently determined, for the first time allowing a functional comparison of TCRs for which the MHC/peptide/TCR structures are known. Extensive amino acid substitutions show that the native Tax residues are optimal at each peptide position. A prominent feature of the TCR contact surface is a deep pocket that accommodates a tyrosine at position 5 of the peptide. For one of these TCRs, this pocket is highly specific for aromatic residues. In the other TCR structure, this pocket is larger, allowing many different residues to be accommodated. The CTL clones also show major differences in the specificity for several other peptide residues, including side chains that are not directly contacted by the TCR. Despite the specificity of these clones, peptides that are distinct at five or six positions from Tax11-19 induce CTL activity, indicating that substantial changes of the peptide surface are tolerated. Human peptides with limited sequence homology to Tax11-19 represent partial TCR agonists for these CTL clones. The distinct functional properties of these CTL clones highlight structural features that determine TCR specificity and cross-reactivity for MHC-bound peptides.

Published

1999

3. CD8+ myelin peptide-specific T cells can chemoattract CD4+ myelin peptide-specific T cells: importance of IFN-inducible protein 10

Author

W E, Biddison, W W, Cruikshank, D M, Center, C M, Pelfrey, D D, Taub, and R V, Turner

Subjects

CD4-Positive T-Lymphocytes, Multiple Sclerosis, Molecular Sequence Data, Myelin Basic Protein, CD8-Positive T-Lymphocytes, Chemokine CXCL10, Chemotaxis, Leukocyte, Cytokines, Humans, Amino Acid Sequence, Chemokines, Myelin Proteolipid Protein, Peptides, Chemokines, CXC, Cells, Cultured

Abstract

The demyelination process that occurs in the central nervous system (CNS) of patients with multiple sclerosis (MS) is due, in part, to an inflammatory response in which CD4+ and CD8+ T cells and macrophages infiltrate white matter. While it is thought that the inflammatory and demyelination process in MS is the product of Th1-associated cytokines secreted by CD4+ myelin protein-specific T cells present in the CNS, the mechanisms that are responsible for the recruitment and maintenance of these myelin-reactive CD4+ T cells in the CNS have not been elucidated. We have shown previously that CD8+ CTL that recognize peptides derived from sequences of the myelin proteolipid protein (PLP) presented by HLA class I molecules can be generated in vitro, and that these PLP-specific CD8+ CTL secrete the proinflammatory chemokines macrophage-inflammatory protein-1alpha and -1beta, IL-16, and IP-10. In this study, we demonstrate that soluble products of these PLP-specific CD8+ CTL can chemoattract CD4+ T cells that are specific for a myelin basic protein peptide and a PLP peptide, and that the majority of this chemotactic activity is mediated by IFN-inducible protein 10. These results demonstrate that PLP-specific CD8+ T cells can play a role in the recruitment and retention of myelin-derived peptide-specific CD4+ T cells, and indicate that they may play a proinflammatory role in the pathogenesis of MS.

Published

1998

4. C2H2-546: a zinc finger protein differentially expressed in HTLV-1 infected T cells

Author

P D, Drew, A M, Gado, R D, Canning, J W, Nagle, A M, Dehejia, M H, Polymeropoulos, W E, Biddison, S, Jacobson, and K G, Becker

Subjects

Gene Expression Regulation, Viral, DNA, Complementary, T-Lymphocytes, Molecular Sequence Data, Kruppel-Like Transcription Factors, Saccharomyces cerevisiae, Polymerase Chain Reaction, Species Specificity, Tumor Cells, Cultured, Animals, Humans, Leukemia-Lymphoma, Adult T-Cell, Amino Acid Sequence, Chromosomes, Artificial, Yeast, Mammals, Human T-lymphotropic virus 1, Base Sequence, Chromosomes, Human, Pair 10, Nuclear Proteins, Zinc Fingers, HTLV-I Infections, Paraparesis, Tropical Spastic, Neoplasm Proteins, Drosophila melanogaster, Genes, Transcription Factors

Abstract

We report the cloning and characterization of a novel cDNA termed C2H2-546 which encodes a C2H2-type zinc finger protein. C2H2-546 RNA is expressed in the HTLV-1 infected T cells examined which were derived from HAM-TSP patients, but not in T cells derived from ATL patients. The C2H2-546 gene is conserved in humans and primates and maps to chromosome 10q11.2, a site associated with a variety of cancers. Thus, C2H2-546 is a candidate regulatory molecule important in the formation of these tumors, and may serve as an important marker to distinguish HTLV-1 infected ATL versus HAM-TSP T cell lineages.

Published

1998

5. Assembly, specific binding, and crystallization of a human TCR-alphabeta with an antigenic Tax peptide from human T lymphotropic virus type 1 and the class I MHC molecule HLA-A2

Author

D N, Garboczi, U, Utz, P, Ghosh, A, Seth, J, Kim, E A, VanTienhoven, W E, Biddison, and D C, Wiley

Subjects

Human T-lymphotropic virus 1, Protein Folding, Macromolecular Substances, Protein Conformation, Receptors, Antigen, T-Cell, alpha-beta, Molecular Sequence Data, Gene Products, tax, Crystallography, X-Ray, Structure-Activity Relationship, HLA-A2 Antigen, Humans, Amino Acid Sequence, Disulfides, HTLV-I Antigens, Protein Binding

Abstract

T lymphocytes use TCR-alphabeta to bind and to recognize complexes of antigenic peptides bound to MHC proteins located at the surface of APCs. We have assembled and crystallized this intercellular complex of TCR/peptide/MHC from soluble human TCR-alphabeta and soluble peptide/HLA-A2 complexes. The soluble TCR-alphabeta binds specifically to its in vivo ligand, the complex of HLA-A2, and a peptide from the Tax protein of human T lymphotropic virus type 1. The soluble TCR also binds in vitro to an altered peptide ligand, which appears to be a partial agonist in T cell assays as determined by its ability to elicit different cytolytic and lymphokine secretion responses. Heterodimerization and the antigenic specificity of the TCR do not require its interchain disulfide bond, transmembrane segments, or glycosylations. Crystals of the TCR/peptide/HLA-A2 complex diffract x-rays, providing the means to study in atomic detail the mechanism of Ag-specific cell-cell recognition between T cells and target cells.

Published

1996

6. Binding and presentation of peptides derived from melanoma antigens MART-1 and glycoprotein-100 by HLA-A2 subtypes. Implications for peptide-based immunotherapy

Author

L, Rivoltini, D J, Loftus, K, Barracchini, F, Arienti, A, Mazzocchi, W E, Biddison, M L, Salgaller, E, Appella, G, Parmiani, and F M, Marincola

Subjects

Antigen Presentation, Membrane Glycoproteins, Molecular Sequence Data, Lymphocyte Activation, Immunotherapy, Adoptive, Neoplasm Proteins, MART-1 Antigen, Antigens, Neoplasm, HLA-A2 Antigen, Humans, Amino Acid Sequence, Peptides, Melanoma, Alleles, T-Lymphocytes, Cytotoxic, gp100 Melanoma Antigen

Abstract

Cellular immune responses to melanoma-associated Ags are the focus of ongoing studies aimed at developing immunotherapies for treatment of malignant melanoma. Melanoma predominantly affects Caucasians, a population in whom expression of HLA-A2 is prevalent. Among HLA-A2 subtypes, HLA-A*0201 is widely expressed, and HLA-A*0201-restricted, tumor-reactive CTL responses are well studied. We have observed in a group of melanoma patients an unexpectedly high frequency (approximately 20%) of non-HLA-A*0201 subtypes (*0202, *0204, and *0205), and little is known regarding antimelanoma response profiles in patients expressing such subtypes. We analyzed non-HLA-A*0201 peptide response profiles using HLA-A*0201-restricted epitopes from melanoma Ags MART-1/Melan A and glycoprotein 100. Most of these peptides bound to the majority of subtypes tested with 50% inhibitory concentrations less than 500 nM. Recognition of cells pulsed with different peptides (MART-1(27-35), G9(154), and G9(280) Flu M1(58-66)) and expressing different subtype molecules by HLA-A*0201-restricted CTL was limited to only a subset of non-HLA-A*0201 molecules, and the peptide/subtype complexes recognized varied among the effector populations tested. CTL responses elicited from PBL of patients and healthy donors expressing subtypes HLA-A*0202 and HLA-A*0205 suggested significant differences among HLA-A2 subtype function in the context of melanoma Ag presentation. These observations imply the necessity of subtyping patients considered for peptide-based protocols and highlight the need for further study of melanoma-directed cellular responses among patients expressing non-HLA-A*0201 subtypes.

Published

1996

7. The HLA-B14 peptide binding site can accommodate peptides with different combinations of anchor residues

Author

M, DiBrino, K C, Parker, D H, Margulies, J, Shiloach, R V, Turner, W E, Biddison, and J E, Coligan

Subjects

Alanine, Binding Sites, Base Sequence, Viral Core Proteins, Molecular Sequence Data, Nucleocapsid Proteins, Cell Line, Epitopes, HLA-B14 Antigen, Nucleoproteins, HLA-B Antigens, Influenza A virus, Humans, Amino Acid Sequence, Peptides, DNA Primers, T-Lymphocytes, Cytotoxic

Abstract

Most peptides that bind to a particular major histocompatibility complex class I molecule share amino acid residues important for binding at one or two positions. Sequence analyses of peptides bound to HLA-B14 revealed at least four candidates for these so-called anchor residues: Arg at P2, Tyr at P3, Arg at P5, and Leu at P9. Combinations of any three of these amino acids sufficed for binding to HLA-B14 in vitro. Using this information, we identified an antigenic peptide critical for cytotoxic T lymphocyte recognition of virus-infected cells. Molecular models of HLA-B14 peptide complexes were constructed to investigate how the potential anchor residues might function. By using binding data to calculate the contribution to binding of each amino acid at anchor positions and predicting the stability of all possible nonapeptide complexes that could be formed from antigenic proteins, we estimate that three known antigenic nonapeptides are in the highest affinity cohort of peptides. Thus, even when multiple combinations of anchor residues contribute to binding, antigenic peptides are routinely identifiable.

Published

1994

8. Endogenous peptides with distinct amino acid anchor residue motifs bind to HLA-A1 and HLA-B8

Author

M, DiBrino, K C, Parker, J, Shiloach, R V, Turner, T, Tsuchida, M, Garfield, W E, Biddison, and J E, Coligan

Subjects

Epitopes, Structure-Activity Relationship, Base Sequence, Influenza A virus, Molecular Sequence Data, Humans, Amino Acid Sequence, Peptides, Antigens, Viral, HLA-A1 Antigen, DNA Primers, HLA-B8 Antigen, Protein Binding

Abstract

Distinct amino acid (aa) residue motifs for peptides binding to HLA-A1 and HLA-B8 were identified by sequence analyses of reversed-phase HPLC fractions containing endogenous peptides derived from these HLA molecules. Fifteen different primary sequences were determined for HLA-A1-associated peptides, 12 of which were nine aa in length. Common features among these peptide sequences were Tyr at the COOH-terminus, a negatively charged aa (usually Glu) at position 3 (P3), and Pro at P4. Twenty-seven different primary sequence assignments were made for HLA-B8-associated peptides, most of which were eight aa in length. Lys, and in a few cases Arg, predominated at P3 and P5; Leu and Pro predominated at P2, and Leu was the preferred COOH-terminal residue. Unlike all other human class I molecules whose peptide-binding properties have been studied, both HLA-A1 and HLA-B8 endogenous peptide sequences have a dominant anchor residue at P3, and these aa are opposite in charge to the aa at position 156 of the peptide-binding site. Synthetic peptides corresponding to endogenous peptide sequences bound to their respective HLA molecules in vitro, indicating that they derive from peptides bound to HLA and not from copurifying contaminants. Eight of the HLA-A1 and HLA-B8 endogenous peptide sequences matched intracellularly expressed proteins found in protein sequence data bases. The HLA-A1 peptide-binding motif was then used to identify potential antigenic peptides from influenza A viral proteins that bound to HLA-A1 in vitro.

Published

1994

9. HLA-A1 and HLA-A3 T cell epitopes derived from influenza virus proteins predicted from peptide binding motifs

Author

M, DiBrino, T, Tsuchida, R V, Turner, K C, Parker, J E, Coligan, and W E, Biddison

Subjects

Binding Sites, Viral Core Proteins, Molecular Sequence Data, RNA-Binding Proteins, HLA-A3 Antigen, Nucleocapsid Proteins, Orthomyxoviridae, Peptide Fragments, Epitopes, Viral Proteins, Nucleoproteins, Humans, Amino Acid Sequence, HLA-A1 Antigen, T-Lymphocytes, Cytotoxic

Abstract

The potential value of peptide binding motifs of HLA class I molecules for the prediction of viral epitopes presented to T cells has been analyzed for two common HLA alleles. CTL generated against type A influenza virus recognize peptide epitopes derived from the nucleoprotein (NP) and basic polymerase 1 presented by HLA-A1, and epitopes derived from NP presented by HLA-A3. Distinct peptide binding motifs with characteristic anchor residues were previously identified for each of these class I molecules based on the sequences of endogenous peptides: for HLA-A1, position 3 = Asp or Glu and position 9 = Tyr; for HLA-A3, position 2 = Leu and position 9 = Lys or Tyr. Six peptides containing the HLA-A1 binding motif were identified within the sequences of the NP and basic polymerase 1 proteins, and one peptide containing the HLA-A3 motif was identified in the NP molecule. Three of the six HLA-A1 peptides and the one HLA-A3 NP peptide could bind to HLA-A1 or HLA-A3, respectively, in an in vitro peptide binding assay. Two of the HLA-A1-binding peptides could sensitize target cells for lysis by influenza virus-immune CTL populations restricted by HLA-A1 (NP 44-52 CTELKLSDY and PB1 591-599 VSDGGPNLY), and the one HLA-A3 NP peptide (NP 265-273 ILRGSVAHK) could sensitize target cells for lysis by HLA-A3-restricted influenza-immune CTL. Each peptide was also shown to be able to induce peptide-specific class I-restricted CTL in vitro, and the CTL generated against two of these peptides could specifically recognize virus-infected targets. Thus, these peptide binding motifs can be used to construct immunogenic synthetic epitopes which are capable of inducing antiviral T cell-mediated immune responses.

Published

1993

10. Cytotoxic T cells isolated from ovarian malignant ascites recognize a peptide derived from the HER-2/neu proto-oncogene

Author

Constantin G. Ioannides, W E Biddison, J T Wharton, B Fisk, Catherine A. O'Brian, and Dominic Fan

Subjects

Cellular immunity, Receptor, ErbB-2, Immunology, Molecular Sequence Data, Biology, Proto-Oncogene Mas, Cell Line, Epitopes, Immune system, Antigen, Antigens, Neoplasm, Proto-Oncogene Proteins, HLA-A2 Antigen, Cytotoxic T cell, Humans, Amino Acid Sequence, Peptide sequence, Ovarian Neoplasms, Oncogene, Tumor-infiltrating lymphocytes, Ascites, Peptide Fragments, ErbB Receptors, CTL, Cancer research, Female, T-Lymphocytes, Cytotoxic

Abstract

The HER-2/neu proto-oncogene encodes a transmembrane receptor protein whose expression is enhanced in a number of breast and ovarian tumors and correlates with tumor aggressiveness, suggesting that it may play an important role in tumor growth. Recent evidence suggests that HER-2/neu may be a potential candidate for targeted immune intervention. In this report we show that cytotoxic T lymphocytes (CTL) expanded from tumor-associated lymphocytes with HLA-A2+ and HER-2/neu+ tumors can specifically recognize synthetic peptides corresponding to amino acids 971-980 of HER-2/neu protein. This sequence includes a potential amphiphilic area containing both Rothbard's epitode motifs and HLA-A2 anchor residues. Our study provides the first direct evidence of HER-2/neu-reactive CTL in humans. The fact that these HER-2/neu peptide-reactive CTL show significantly lower reactivity with corresponding EGF-R peptides offers new perspectives for understanding the recognition of self-antigens by tumor-reactive T cells.

Published

1993

11. Sequence motifs important for peptide binding to the human MHC class I molecule, HLA-A2

Author

K C, Parker, M A, Bednarek, L K, Hull, U, Utz, B, Cunningham, H J, Zweerink, W E, Biddison, and J E, Coligan

Subjects

HIV Antigens, Molecular Sequence Data, Glycine, Cytomegalovirus, In Vitro Techniques, Viral Matrix Proteins, Structure-Activity Relationship, Influenza A virus, HLA-A2 Antigen, HIV-1, Humans, Amino Acid Sequence, Peptides, Antigens, Viral

Abstract

Previous studies have indicated that most HLA-A2-binding peptides are 9 amino acid (aa) residues long, with a Leu at position 2 (P2), and a Val or Leu at P9. We compared the binding properties of different peptides by measuring the rate of dissociation of beta 2-microglobulin from peptide-specific HLA-A2 complexes. The simplest peptide that we identified that could form HLA-A2 complexes had the sequence (in single letter aa code) GLFGGGGGV, indicating that three nonglycine aa are sufficient for binding to HLA-A2. To determine whether most nonapeptides that contained Leu at P2 and Val or Leu at P9 could bind to HLA-A2, we tested the binding of nonapeptides selected from published HIV and melanoma protein sequences, and found that six of seven tested formed stable HLA-A2 complexes. We identified an optimal antigenic undecapeptide from the cytomegalovirus gB protein that could form stable HLA-A2 complexes that contained apparent anchor residues at P2 and P11 (sequence FIAGN-SAYEYV), indicating that the spacing between anchor residues can be somewhat variable. Finally, we tested the importance of every aa in the influenza A matrix peptide 58-66 (sequence GILGFVFTL) for binding to HLA-A2, by using Ala-substituted and Lys-substituted peptides. We found that multiple positions were important for stable binding, including P2, P3, P5-P7, and P9. We conclude that the P2 and P9 anchor residues are of prime importance for peptide binding to HLA-A2. However, other peptide side chains (especially at P3) contribute to the stability of the interaction. In certain cases, the optimal length for peptide binding can be longer than 9 residues.

Published

1992

12. Presentation of three different viral peptides, HTLV-1 Tax, HCMV gB, and influenza virus M1, is determined by common structural features of the HLA-A2.1 molecule

Author

U, Utz, S, Koenig, J E, Coligan, and W E, Biddison

Subjects

Cytotoxicity, Immunologic, Human T-lymphotropic virus 1, Binding Sites, Molecular Sequence Data, Antigen-Presenting Cells, Gene Products, tax, Viral Matrix Proteins, Structure-Activity Relationship, Viral Envelope Proteins, HLA-A2 Antigen, Mutagenesis, Site-Directed, Humans, Amino Acid Sequence, Peptides, Antigens, Viral

Abstract

To determine whether similar or dissimilar molecular features of class I molecules are involved in the presentation of structurally distinct peptides, we have investigated the influence of different pockets of the HLA-A2.1 molecule on the presentation of three different viral peptides. HTLV-I Tax peptide 12-19, HCMV gB 619-628, and influenza M1 58-66 are minimal peptides that induce HLA-A2.1-restricted noncross-reactive CTL. A detailed analysis of the structural features of HLA-A2.1 that are involved in peptide presentation was undertaken using a panel of 11 HLA-A2 mutants with single amino acid substitutions within pockets present in the peptide binding site. Nine of the 11 mutants affected presentation of each of the three peptides, whereas the other two mutants had negative effects on presentation of only two of these viral peptides. These results indicate that common structural features in HLA-A2 determine the binding of different peptides, and help to provide a plausible explanation for how structurally diverse peptides bind to HLA-A2.

Published

1992

13. Peptide binding to HLA-A2 and HLA-B27 isolated from Escherichia coli. Reconstitution of HLA-A2 and HLA-B27 heavy chain/beta 2-microglobulin complexes requires specific peptides

Author

K C, Parker, B M, Carreno, L, Sestak, U, Utz, W E, Biddison, and J E, Coligan

Subjects

Base Sequence, Macromolecular Substances, Molecular Sequence Data, Antibodies, Monoclonal, Polymerase Chain Reaction, Recombinant Proteins, Oligodeoxyribonucleotides, HLA-A2 Antigen, Escherichia coli, Humans, Amino Acid Sequence, Cloning, Molecular, Peptides, beta 2-Microglobulin, HLA-B27 Antigen, Plasmids, Protein Binding

Abstract

The specificity of peptide binding by human leukocyte antigen (HLA) class I molecules was investigated in a cell-free direct-binding assay. Peptides were assessed for binding to HLA-A2 and HLA-B27 by measuring the formation of heterotrimeric HLA complexes that consisted of iodinated beta 2-microglobulin, HLA heavy chain fragments isolated from the Escherichia coli cytoplasm, and peptide. In this system, no detectable HLA heavy chain-beta 2-microglobulin complexes were formed unless appropriate peptides were intentionally added to the reconstitution solution. Analysis with monoclonal antibodies demonstrated that these heterotrimeric complexes were correctly folded. Five nonhomologous peptides, known to form complexes with HLA-A2 or HLA-B27 from T-cell functional studies, were tested for their capacity to bind to HLA-A2 and HLA-B27 using the reconstitution assay. Four of the peptides bound to the appropriate class I molecule only. One peptide and some (but not all) substitution analogs of it bound to both HLA-A2 and HLA-B27. The effect of peptide length on binding to HLA-B27 was studied, and it was found that the optimal length was 9 or 10 amino acid residues; however, one peptide that bound to HLA-B27 was 15 amino acids long. All peptides that bound to HLA-B27 in the direct-binding assay also competed with antigenic peptides for binding to HLA-B27 on the surface of intact cells, as determined by a standard cytotoxic T-lymphocyte functional assay. Thus, we conclude that HLA-A2 and HLA-B27 bind distinct but partially overlapping sets of peptides and that, at least in vitro, the assembly of HLA heavy chain-beta 2-microglobulin complexes requires specific peptides.

Published

1992

14. Overlapping epitopes that are recognized by CD8+ HLA class I-restricted and CD4+ class II-restricted cytotoxic T lymphocytes are contained within an influenza nucleoprotein peptide

Author

B M, Carreno, R V, Turner, W E, Biddison, and J E, Coligan

Subjects

CD4-Positive T-Lymphocytes, Cytotoxicity, Immunologic, HLA-D Antigens, Immunity, Cellular, CD8 Antigens, Viral Core Proteins, Histocompatibility Antigens Class I, Molecular Sequence Data, In Vitro Techniques, Nucleocapsid Proteins, Epitopes, Viral Proteins, Nucleoproteins, Influenza A virus, T-Lymphocyte Subsets, Humans, Amino Acid Sequence, T-Lymphocytes, Cytotoxic

Abstract

Viral epitopes that are recognized by both HLA class I-restricted and class II-restricted T cells have been defined for a type A influenza virus nucleoprotein (NP) peptide. CD8+ and CD4+ CTL lines have been generated against a synthetic peptide encompassing residues 335 to 349 of NP that are restricted by HLA-B37 and HLA-DQw5, respectively. Both of these CTL populations were capable of specifically lysing influenza A virus-infected targets, indicating that a naturally processed NP peptide(s) was being mimicked by the NP (335-349) peptide. Amino acid residues that are critical for recognition of this NP determinant in the context of HLA-B37 and HLA-DQw5 were investigated by the use of panels of truncated and alanine-substituted NP peptides. The results demonstrate that: 1) truncations in the amino- or carboxy-terminal ends differentially affect CD8+ and CD4+ CTL recognition; 2) the NP (335-349) sequence contains two octapeptide epitopes that share a core of six amino acid residues (NP 338-343); and 3) alanine substitutions at five of these residues abrogated recognition by at least one of the CD8+ and CD4+ CTL lines. Thus, these class I- and class II-restricted CTL lines recognize similar but distinct epitopes, and different structural features of the NP peptide are required for presentation by HLA-B37 and HLA-DQw5. Comparison of the amino acid sequences of the NP peptide presented by HLA-B37 and HLA-DQw5 with other peptides known to be presented by both class I and class II molecules revealed a common motif among these peptides.

Published

1992

15. The 45 pocket of HLA-A2.1 plays a role in presentation of influenza virus matrix peptide and alloantigens

Author

C C, Winter, B M, Carreno, R V, Turner, S, Koenig, and W E, Biddison

Subjects

Models, Molecular, Viral Matrix Proteins, Isoantigens, Structure-Activity Relationship, Base Sequence, HLA-A Antigens, Influenza A virus, Molecular Sequence Data, Mutation, Humans, Gene Products, tax, Transfection, T-Lymphocytes, Cytotoxic

Abstract

Amino acid substitutions were introduced into the 45 pocket of HLA-A2.1 to determine the potential role of this structurally defined feature of class I molecules in viral peptide and alloantigen presentation. The 45 pocket lies below the alpha 1-domain alpha-helix and is composed of five amino acids, three of which differ between HLA-A2.1 and HLA-B37. These two class I molecules have previously been shown to have largely non-overlapping peptide-binding specificities. Site-directed mutagenesis was used to replace the hydrophobic residues at positions 24, 45, and 67 in the 45 pocket of HLA-A2.1 with the hydrophilic amino acids found in these positions in HLA-B37. Thus, three single amino acid mutants were produced: 24A----S, 45 M----T, and 67V----S. These mutants were transfected into HMy2.C1R cells and assessed for their ability to present influenza virus matrix M1 57-68 peptide and HTLV-I Tax-1 2-25 peptide to HLA-A2.1-restricted, peptide-specific CTL and to present alloantigens to HLA-A2-allospecific CTL lines. Each of these substitutions in the 45 pocket produced a molecule that failed to present the M1 peptide to most M1 peptide-specific CTL lines. In contrast, none of these mutations affected presentation of the Tax-1 peptide to Tax-1-specific CTL lines, which indicates that these mutant HLA-A2 molecules can function in viral peptide presentation. Two of the three substitutions in the 45 pocket resulted in lack of recognition by a subset of HLA-A2 allospecific CTL lines. These results demonstrate that the amino acid side chains in the 45 pocket can strongly influence peptide presentation and suggest that the 45 pocket may play a role in determining peptide-binding specificity.

Published

1991

16. Specificity of peptide binding by the HLA-A2.1 molecule

Author

N, Shimojo, W L, Maloy, R W, Anderson, W E, Biddison, and J E, Coligan

Subjects

Rotavirus, Binding Sites, HLA-A Antigens, Molecular Sequence Data, Antigen-Presenting Cells, Binding, Competitive, Viral Matrix Proteins, Structure-Activity Relationship, Influenza A virus, Humans, Amino Acid Sequence, Antigens, Viral, Oligopeptides, T-Lymphocytes, Cytotoxic

Abstract

The HLA-A2 molecule contains a putative peptide binding site that is bounded by two alpha-helices and a beta-pleated sheet floor. Previous studies have demonstrated that the influenza virus matrix peptide M1 55-73 can sensitize target cells for lysis by HLA-A2.1-restricted virus-immune CTL and can induce CTL that can lyse virus-infected target cells. To assess the specificity of peptide binding by the HLA-A2.1 molecule, we examined the ability of seven variant M1 peptides to be recognized by a panel of M1 55-73 peptide-specific HLA-A2.1-restricted CTL lines. The results demonstrate that five out of the seven variant M1 55-73 peptides could be recognized by A2.1-restricted M1 55-73 peptide-specific CTL lines. The two variant peptides that were not recognized by any CTL could bind to HLA-A2.1 as indicated by their ability to compete for presentation of the M1 55-73 peptide. In addition, 5 of a panel of 24 unrelated peptides tested could also compete for M1 55-73 presentation by HLA-A2.1. One peptide derived from the sequence of a rotavirus protein could sensitize HLA-A2.1+ targets for lysis by M1 55-73 peptide-specific CTL. We conclude from these studies that: 1) the HLA-A2.1 molecule can bind a broad spectrum of peptides; 2) T cells selected for the ability to recognize one peptide plus a class I molecule can actually recognize an unrelated peptide presented by that same class I molecule; and 3) a stretch of three adjacent hydrophobic amino acids may be an important common feature of peptides that can bind to HLA-A2.1.

Published

1989

17. Analysis of the molecular basis of HLA-A3 recognition by cytotoxic T cells using defined mutants of the HLA-A3 molecule

Author

M L, Jelachich, E P, Cowan, R V, Turner, J E, Coligan, and W E, Biddison

Subjects

Adult, Molecular Sequence Data, Fibroblasts, HLA-A3 Antigen, Cytotoxicity Tests, Immunologic, Epitopes, Mice, Structure-Activity Relationship, Genes, HLA Antigens, Influenza A virus, Mutation, Animals, Humans, Amino Acid Sequence, Cell Line, Transformed, T-Lymphocytes, Cytotoxic

Abstract

The structure-function relationships in human class I HLA molecules have been examined by the analysis of two T cell-defined subtypes of HLA-A3 (A3.1 and A3.2). These subtypes differ by two amino acid residues that are located at positions 152 (GluA3.1 vs ValA3.2) and 156 (LeuA3.1 vs GlnA3.2). By the methods of site-directed mutagenesis and DNA-mediated gene transfer, mammalian cell transfectants have been produced that express only one of the above A3.2 amino acid residues at either position 152 or position 156. Previous studies using murine transfectants have shown that A3.1- and A3.2-expressing cells can be distinguished by A3.1-restricted type A influenza virus-specific CTL and A3.2-allospecific CTL and have implied that amino acid position 152 plays a key role in this specificity. To test whether these results were a function of the virus specificity, the alloantigen, or the cell type expressing the class I molecules, we have tested the recognition of human and murine cell transfectants by A3.1-restricted, A/JAP/305/57 and B/Ann Arbor-specific CTL and by A3.1- and A3.2-allospecific CTL. The results indicate that the Glu at position 152 is critical for recognition by all of the A3.1-restricted CTL populations tested and 15 of 16 of the A3.1-allospecific CTL populations tested. The A3.1 Leu at position 156 was sufficient for recognition by only one A3.1-allospecific CTL line. Substitution of the charged Glu residue for the polar Gln at position 156 of A3.2 affected recognition of some but not all A3.2-alloreactive CTL. These data demonstrate that the structural basis for epitopes that are recognized by almost all CTL that discriminate between A3.1 and A3.2 is primarily the amino acid at position 152. The implications of these data for Ag presentation and CTL recognition are discussed.

Published

1988