FLOW-CYTOMETRIC DETERMINATION OF PEPTIDE CLASS-I COMPLEX-FORMATION - IDENTIFICATION OF P53 PEPTIDES THAT BIND TO HLA-A2

被引：71

作者：

ZEH, HJ

LEDER, GH

LOTZE, MT

SALTER, RD

TECTOR, M

STUBER, G

MODROW, S

STORKUS, WJ

机构：

[1] UNIV PITTSBURGH,SCH MED,DEPT SURG,PITTSBURGH,PA 15261

[2] UNIV PITTSBURGH,DEPT MOLEC GENET & BIOCHEM,PITTSBURGH,PA

[3] UNIV PITTSBURGH,DEPT PATHOL,PITTSBURGH,PA

[4] KAROLINSKA INST,DEPT TUMOR BIOL,KAROLINSKA,SWEDEN

[5] UNIV REGENSBURG,INST MED MICROBIOL,W-8400 REGENSBURG,GERMANY

来源：

HUMAN IMMUNOLOGY | 1994年 / 39卷 / 02期

关键词：

D O I：

10.1016/0198-8859(94)90105-8

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

A novel class I-peptide-binding assay was developed and used to identify a series of peptides derived from the human p53 tumor-suppressor gene product capable of binding the HLA-A2 class I allele. Brief pH 3.3 acid treatment of human cell lines rapidly denatures preexisting class I complexes, as detected by loss of binding of conformation-dependent mAbs, leaving only free class I heavy chains associated with the viable cell surface. These heavy chains may be induced to refold and be recognized by antibodies (in 2-4 hours) when acid-treated cells are coincubated with exogenous beta(2)-microglobulin and peptides capable of binding the relevant class I allele examined. This assay, with a detection limit of 1-10 nM peptide, was used to screen the capacity of a panel of nine peptides bearing HLA-A2-binding motifs and derived from the human p53 tumor-suppressor protein sequence. Eight of the nine peptides bound to, and reconstituted, HLA-A2 on acid-treated cells. This assay system will enable the rapid identification of peptides binding to any class I allele, which is the initial prerequisite for elucidating potential CD8 + T-cell epitopes.

引用

页码：79 / 86

页数：8

共 35 条

[1] PUTTING TOGETHER AN MHC CLASS-I MOLECULE
BIJLMAKERS, MJ
PLOEGH, HL
[J]. CURRENT OPINION IN IMMUNOLOGY, 1993, 5 (01) : 21 - 26
[2] STRUCTURE OF THE HUMAN CLASS-I HISTOCOMPATIBILITY ANTIGEN, HLA-A2
BJORKMAN, PJ
SAPER, MA
SAMRAOUI, B
BENNETT, WS
STROMINGER, JL
WILEY, DC
[J]. NATURE, 1987, 329 (6139) : 506 - 512
[3] TOWARD A GENETIC-ANALYSIS OF TUMOR REJECTION ANTIGENS
BOON, T
[J]. ADVANCES IN CANCER RESEARCH, 1992, 58 : 177 - 210
[4] ANTIGEN PRESENTATION - STRUCTURAL THEMES AND FUNCTIONAL VARIATIONS
BRACIALE, TJ
BRACIALE, VL
[J]. IMMUNOLOGY TODAY, 1991, 12 (04): : 124 - 129
[5] PRESENTATION OF VIRAL-ANTIGEN CONTROLLED BY A GENE IN THE MAJOR HISTOCOMPATIBILITY COMPLEX
CERUNDOLO, V
ALEXANDER, J
ANDERSON, K
LAMB, C
CRESSWELL, P
MCMICHAEL, A
GOTCH, F
TOWNSEND, A
[J]. NATURE, 1990, 345 (6274) : 449 - 452
[6] THE BINDING-AFFINITY AND DISSOCIATION RATES OF PEPTIDES FOR CLASS-I MAJOR HISTOCOMPATIBILITY COMPLEX-MOLECULES
CERUNDOLO, V
ELLIOTT, T
ELVIN, J
BASTIN, J
RAMMENSEE, HG
TOWNSEND, A
[J]. EUROPEAN JOURNAL OF IMMUNOLOGY, 1991, 21 (09) : 2069 - 2075
[7] AN ANTIGENIC PEPTIDE OF THE HIV-1 NEF PROTEIN RECOGNIZED BY CYTOTOXIC LYMPHOCYTE-T OF SEROPOSITIVE INDIVIDUALS IN ASSOCIATION WITH DIFFERENT HLA-B MOLECULES
CULMANN, B
GOMARD, E
KIENY, MP
GUY, B
DREYFUS, F
SAIMOT, AG
SERENI, D
LEVY, JP
[J]. EUROPEAN JOURNAL OF IMMUNOLOGY, 1989, 19 (12) : 2383 - 2386
[8] A METHOD TO QUANTIFY BINDING OF UNLABELED PEPTIDES TO CLASS-I MHC MOLECULES AND DETECT THEIR ALLELE SPECIFICITY
ELVIN, J
POTTER, C
ELLIOTT, T
CERUNDOLO, V
TOWNSEND, A
[J]. JOURNAL OF IMMUNOLOGICAL METHODS, 1993, 158 (02) : 161 - 171
[9] 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
[10] P53 MUTATIONS IN HUMAN CANCERS
HOLLSTEIN, M
SIDRANSKY, D
VOGELSTEIN, B
HARRIS, CC
[J]. SCIENCE, 1991, 253 (5015) : 49 - 53

← 1 2 3 4 →