SPECIFIC BINDING OF LEUKEMIA ONCOGENE FUSION PROTEIN-PEPTIDES TO HLA CLASS-I MOLECULES

被引:157
作者
BOCCHIA, M
WENTWORTH, PA
SOUTHWOOD, S
SIDNEY, J
MCGRAW, K
SCHEINBERG, DA
SETTE, A
机构
[1] MEM SLOAN KETTERING CANC CTR,NEW YORK,NY 10021
[2] CYTEL CORP,SAN DIEGO,CA 92121
来源
BLOOD | 1995年 / 85卷 / 10期
关键词
D O I
10.1182/blood.V85.10.2680.bloodjournal85102680
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Many human leukemias are characterized by chromosomal translocations yielding hybrid RNAs capable of encoding fusion chimeric proteins. The unique amino acid sequences found in these oncogenic fusion proteins represent true tumor-specific antigens that are potentially immunogenic. Although these leukemia-specific fusion proteins have an intracellular location, they might be recognized immunologically by T lymphocytes if peptides derived from the unique sequences are capable of presentation by the major histocompatibility complex (MHC) molecules on leukemic cells. The ability of a series of synthetic peptides corresponding to the junctional sequences of chronic myelogenous leukemia (CML)-derived bcr-abl and acute promyelocytic leukemia (APL)-derived PML-RAR alpha fusion proteins to bind to purified class I molecules was studied. A series of 152 peptides 8, 9, 10, and 11 amino acids in length, spanning the b3a2 and b2a2 breakpoints for CML and PML-RAR alpha A and B breakpoints for APL were analyzed for HLA A1, A2.1, A3.2, A11, A24, B7, B8, and B27 binding motifs. Twenty-one CML peptides and 4 APL peptides were predicted to be potential HLA class I binders. The peptides were tested for binding to appropriate purified HLA molecules in a competition radioimmunoassay. Four peptides derived from b3a2 CML breakpoint bound with high (<50 nmol/L) or intermediate (less than or equal to 500 nmol/L) affinity to HLA A3, A11, and B8. None of the CML b2a2 or PML-RAR alpha A or B junctional peptides showed affinity of this magnitude for the HLA class I molecules tested. This is the first evidence that tumor-specific breakpoint peptides can bind human MHC class I molecules and provides a rationale for developing a therapeutic vaccine strategy. (C) 1995 by The American Society of Hematology.
引用
收藏
页码:2680 / 2684
页数:5
相关论文
共 28 条
  • [1] ANTIN JH, 1993, BLOOD, V82, P2273
  • [2] ANTIGEN PRESENTATION - STRUCTURAL THEMES AND FUNCTIONAL VARIATIONS
    BRACIALE, TJ
    BRACIALE, VL
    [J]. IMMUNOLOGY TODAY, 1991, 12 (04): : 124 - 129
  • [3] 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
  • [4] T-CELL IMMUNITY TO THE JOINING REGION OF P210BCR-ABL PROTEIN
    CHEN, W
    PEACE, DJ
    ROVIRA, DK
    YOU, SG
    CHEEVER, MA
    [J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (04) : 1468 - 1472
  • [5] CULLIS JO, 1994, LEUKEMIA, V8, P165
  • [6] THE T(15-17) TRANSLOCATION OF ACUTE PROMYELOCYTIC LEUKEMIA FUSES THE RETINOIC ACID RECEPTOR-ALPHA GENE TO A NOVEL TRANSCRIBED LOCUS
    DETHE, H
    CHOMIENNE, C
    LANOTTE, M
    DEGOS, L
    DEJEAN, A
    [J]. NATURE, 1990, 347 (6293) : 558 - 561
  • [7] PEPTIDE SELECTION BY CLASS-I MOLECULES OF THE MAJOR HISTOCOMPATIBILITY COMPLEX
    ELLIOTT, T
    SMITH, M
    DRISCOLL, P
    MCMICHAEL, A
    [J]. CURRENT BIOLOGY, 1993, 3 (12) : 854 - 866
  • [8] STRUCTURE OF PEPTIDES ASSOCIATED WITH CLASS-I AND CLASS-II MHC MOLECULES
    ENGELHARD, VH
    [J]. ANNUAL REVIEW OF IMMUNOLOGY, 1994, 12 : 181 - 207
  • [9] ENGLEHARD VH, 1994, CURR OPIN IMMUNOL, V6, P13
  • [10] ALLELE-SPECIFIC MOTIFS REVEALED BY SEQUENCING OF SELF-PEPTIDES ELUTED FROM MHC MOLECULES
    FALK, K
    ROTZSCHKE, O
    STEVANOVIC, S
    JUNG, G
    RAMMENSEE, HG
    [J]. NATURE, 1991, 351 (6324) : 290 - 296
123