IMMUNIZATION AGAINST TUMOR AND MINOR HISTOCOMPATIBILITY ANTIGENS BY ELUTED CELLULAR PEPTIDES LOADED ON ANTIGEN-PROCESSING DEFECTIVE CELLS

被引：40

作者：

FRANKSSON, L

PETERSSON, M

KIESSLING, R

KARRE, K

机构：

[1] KAROLINSKA INST, TUMOR BIOL LAB, CTR MICROBIOL & TUMOR BIOL, BOX 60400, S-10401 STOCKHOLM 60, SWEDEN

[2] KAROLINSKA INST, IMMUNOL LAB, S-10401 STOCKHOLM 60, SWEDEN

来源：

EUROPEAN JOURNAL OF IMMUNOLOGY | 1993年 / 23卷 / 10期

关键词：

ACID ELUTION; CELLULAR ANTIGENS; CYTOTOXIC T-LYMPHOCYTES; PEPTIDE IMMUNIZATION; RMA-S CELLS;

D O I：

10.1002/eji.1830231034

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Material eluted from RMA lymphoma or B6 spleen cells under acid conditions was fractionated by reverse phase high-performance liquid chromatography, and tested for ability to restore the sensitivity to cytotoxic T lymphocytes of the processing/presentation defective mutant line RMA-S. This allowed identification of three fractions (termed M1, M2 and M3) carrying B6 antigens recognized by cytotoxic T lymphocytes (CTL) elicited across the minor histocompatibility barrier A.BY anti-B6 (both H-2b) and one fraction (termed T1) carrying a tumor antigen recognized by B6 anti-RMA CTL. By parallel runs of material from cell lysates over major histocompatibility complex class I affinity columns, the M2 and M3 antigens were defined as K(b) restricted, and M1 and T1 as D(b) restricted. Isolated fractions loaded onto RMA-S cells could be used to prime anti-minor histocompatibility antigen and tumor CTL in vivo. They could also be used for in vitro restimulation of spleen cells from mice that had been primed either by antigen-loaded RMA-S, or by wild-type RMA tumor cells and B6 splenocytes. The CTL generated by these methods were specific for the loading antigen, and they also recognized the antigen on the ''physiological'' target, i.e. RMA or B6 lymphoblasts. This system based on RMA-S as an immunization and target antigen reporter cell may be used for dissection of complex CTL responses, e.g. in studies of clonal composition and epitope dominance, or for studies of tumors that are poor stimulators of immunity.

引用

页码：2606 / 2613

页数：8

共 55 条

[31] OHLEN C, 1990, J IMMUNOL, V145, P52
[32] RESTORATION OF ANTIGEN PRESENTATION TO THE MUTANT-CELL LINE RMA-S BY AN MHC-LINKED TRANSPORTER
POWIS, SJ
TOWNSEND, ARM
DEVERSON, EV
BASTIN, J
BUTCHER, GW
HOWARD, JC
[J]. NATURE, 1991, 354 (6354) : 528 - 531
[33] EFFECT OF POLYMORPHISM OF AN MHC-LINKED TRANSPORTER ON THE PEPTIDES ASSEMBLED IN A CLASS-I MOLECULE
POWIS, SJ
DEVERSON, EV
COADWELL, WJ
CIRUELA, A
HUSKISSON, NS
SMITH, H
BUTCHER, GW
HOWARD, JC
[J]. NATURE, 1992, 357 (6375) : 211 - 215
[34] ROGERS MJ, 1984, J IMMUNOL, V132, P3211
[35] CHARACTERIZATION OF NATURALLY-OCCURRING MINOR HISTOCOMPATIBILITY PEPTIDES INCLUDING H-4 AND H-Y
ROTZSCHKE, O
FALK, K
WALLNY, HJ
FAATH, S
RAMMENSEE, HG
[J]. SCIENCE, 1990, 249 (4966) : 283 - 287
[36] ON THE NATURE OF PEPTIDES INVOLVED IN T-CELL ALLOREACTIVITY
ROTZSCHKE, O
FALK, K
FAATH, S
RAMMENSEE, HG
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1991, 174 (05) : 1059 - 1071
[37] ISOLATION AND ANALYSIS OF NATURALLY PROCESSED VIRAL PEPTIDES AS RECOGNIZED BY CYTOTOXIC T-CELLS
ROTZSCHKE, O
FALK, K
DERES, K
SCHILD, H
NORDA, M
METZGER, J
JUNG, G
RAMMENSEE, HG
[J]. NATURE, 1990, 348 (6298) : 252 - 254
[38] PEPTIDE-INDUCED ANTIVIRAL PROTECTION BY CYTOTOXIC T-CELLS
SCHULZ, M
ZINKERNAGEL, RM
HENGARTNER, H
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (03) : 991 - 993
[39] RESTORED EXPRESSION OF MAJOR HISTOCOMPATIBILITY CLASS-I MOLECULES BY GENE-TRANSFER OF A PUTATIVE PEPTIDE TRANSPORTER
SPIES, T
DEMARS, R
[J]. NATURE, 1991, 351 (6324) : 323 - 324
[40] PRESENTATION OF VIRAL-ANTIGEN BY MHC CLASS-I MOLECULES IS DEPENDENT ON A PUTATIVE PEPTIDE TRANSPORTER HETERODIMER
SPIES, T
CERUNDOLO, V
COLONNA, M
CRESSWELL, P
TOWNSEND, A
DEMARS, R
[J]. NATURE, 1992, 355 (6361) : 644 - 646

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