IDENTIFICATION OF POTENTIAL CTL EPITOPES OF TUMOR-ASSOCIATED ANTIGEN MAGE-1 FOR 5 COMMON HLA-A ALLELES

被引：62

作者：

CELIS, E

FIKES, J

WENTWORTH, P

SIDNEY, J

SOUTHWOOD, S

MAEWAL, A

DELGUERCIO, MF

SETTE, A

LIVINGSTON, B

机构：

[1] Cytel Corporation, San Diego, CA 92121

来源：

MOLECULAR IMMUNOLOGY | 1994年 / 31卷 / 18期

关键词：

TUMOR ANTIGEN; CYTOTOXIC T LYMPHOCYTES; MAGE-1; PEPTIDE HLA INTERACTIONS;

D O I：

10.1016/0161-5890(94)90158-9

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Identification of CTL epitopes for tumor-specific responses is important for the development of immunotherapies to treat cancer patients. We have developed a strategy to identify potential CTL epitopes based on screening of sequences of target proteins for presence of specific motifs recognized by the most common HLA-A alleles, and identification of high affinity binding peptides using in vitro quantitative assays. A systematic analysis using the sequence of the product of the tumor-associated MAGE-1 gene has been carried out. All possible peptides of nine and ten residues, containing binding motifs for HLA-A1, -A2.1, A-3.2, -A11 and -A24 were synthesized and tested for binding using a quantitative assay. Out of 237 possible peptide/MHC combinations, 47 cases demonstrated good binding affinity (K-d less than or equal to 500 nM). Several peptides were identified as good MHC binders for each one of the five HLA-A alleles studied (five for HLA-A1, 11 for HLA-A2.1, 10 for HLA-A3.2, 16 for HLA-A11 and five for HLA-A24. Furthermore, eight of these peptides were found to bind well to more than one HLA-A allele. These results have important implications for the development of immunotherapeutic vaccines to treat malignant melanoma.

引用

页码：1423 / 1430

页数：8

共 28 条

[1] SYNTHETIC PEPTIDES AS VACCINES
ARNON, R
HORWITZ, RJ
[J]. CURRENT OPINION IN IMMUNOLOGY, 1992, 4 (04) : 449 - 453
[2] PRODUCTION OF MONOCLONAL ANTIBODIES TO GROUP-A ERYTHROCYTES, HLA AND OTHER HUMAN CELL-SURFACE ANTIGENS - NEW TOOLS FOR GENETIC-ANALYSIS
BARNSTABLE, CJ
BODMER, WF
BROWN, G
GALFRE, G
MILSTEIN, C
WILLIAMS, AF
ZIEGLER, A
[J]. CELL, 1978, 14 (01) : 9 - 20
[3] MONOCLONAL-ANTIBODY TO HLA-A3
BERGER, AE
DAVIS, JE
CRESSWELL, P
[J]. HYBRIDOMA, 1982, 1 (02): : 87 - 90
[4] PUTTING TOGETHER AN MHC CLASS-I MOLECULE
BIJLMAKERS, MJ
PLOEGH, HL
[J]. CURRENT OPINION IN IMMUNOLOGY, 1993, 5 (01) : 21 - 26
[5] TOWARD A GENETIC-ANALYSIS OF TUMOR REJECTION ANTIGENS
BOON, T
[J]. ADVANCES IN CANCER RESEARCH, 1992, 58 : 177 - 210
[6] INDUCTION OF ANTITUMOR CYTOTOXIC T-LYMPHOCYTES IN NORMAL HUMANS USING PRIMARY CULTURES AND SYNTHETIC PEPTIDE EPITOPES
CELIS, E
TSAI, V
CRIMI, C
DEMARS, R
WENTWORTH, PA
CHESNUT, RW
GREY, HM
SETTE, A
SERRA, HM
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (06) : 2105 - 2109
[7] SEQUENCE AND EXPRESSION PATTERN OF THE HUMAN MAGE2 GENE
DESMET, C
LURQUIN, C
VANDERBRUGGEN, P
DEPLAEN, E
BRASSEUR, F
BOON, T
[J]. IMMUNOGENETICS, 1994, 39 (02) : 121 - 129
[8] DIBRINO M, 1993, J IMMUNOL, V151, P5930
[9] ENDOGENOUS PEPTIDES BOUND TO HLA-A3 POSSESS A SPECIFIC COMBINATION OF ANCHOR RESIDUES THAT PERMIT IDENTIFICATION OF POTENTIAL ANTIGENIC PEPTIDES
DIBRINO, M
PARKER, KC
SHILOACH, J
KNIERMAN, M
LUKSZO, J
TURNER, RV
BIDDISON, WE
COLIGAN, JE
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (04) : 1508 - 1512
[10] THE BIOCHEMISTRY AND CELL BIOLOGY OF ANTIGEN PROCESSING AND PRESENTATION
GERMAIN, RN
MARGULIES, DH
[J]. ANNUAL REVIEW OF IMMUNOLOGY, 1993, 11 : 403 - 450

← 1 2 3 →