CYTOTOXIC T-CELL ACTIVITY ANTAGONIZED BY NATURALLY-OCCURRING HIV-1 GAG VARIANTS

被引：398

作者：

KLENERMAN, P

ROWLANDJONES, S

MCADAM, S

EDWARDS, J

DAENKE, S

LALLOO, D

KOPPE, B

ROSENBERG, W

BOYD, D

EDWARDS, A

GIANGRANDE, P

PHILLIPS, RE

MCMICHAEL, AJ

机构：

[1] UNIV OXFORD,INST MOLEC MED,OXFORD OX3 9DU,ENGLAND

[2] RADCLIFFE INFIRM,DEPT GENITOURINARY MED,OXFORD OX3 7LJ,ENGLAND

[3] CHURCHILL HOSP,OXFORD HAEMOPHILIA CTR,OXFORD OX3 7LV,ENGLAND

来源：

NATURE | 1994年 / 369卷 / 6479期

基金：

英国惠康基金;

关键词：

D O I：

10.1038/369403a0

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

MOST asymptomatic individuals infected with HIV-1 have a cytotoxic T lymphocyte (CTL) response to the virus Gag proteins which can be demonstrated in vitro(1,2). Epitopes have been mapped in p17 Gag and p24 Gag restricted by HLA-B8 (p17-3 and p24-13) and -B27 (p24-14)(2,3). Viruses isolated from patients who make CTL responses to these peptides vary within the genetic sequences encoding these epitopes and some mutations lead to reduction in killing activity in vitro(4). This mas attributed to either failure of the variant epitope to bind major histocompatibility complex class I or failure of T-cell receptors to bind the presented peptide. But peptide variants of class I-restricted epitopes cause 'antagonism', that is, the presence of a variant epitope (in the form of peptide) inhibits normal lysis of targets presenting the original epitope(5,6). This mirrors similar findings in class II-restricted systems(7-10). Here we report that naturally occurring variant forms of p17-3, p24-13 and p24-14 may cause antagonism of CTL lines derived from the same individuals. The effect is present if the epitopes are derived from synthetic peptides and when they are processed from full-length proteins expressed by either recombinant vaccinia constructs or replicating HIV.

引用

页码：403 / 407

页数：5

共 18 条

[1] ANTIGEN ANALOG MAJOR HISTOCOMPATIBILITY COMPLEXES ACT AS ANTAGONISTS OF THE T-CELL RECEPTOR
DEMAGISTRIS, MT
ALEXANDER, J
COGGESHALL, M
ALTMAN, A
GAETA, FCA
GREY, HM
SETTE, A
[J]. CELL, 1992, 68 (04) : 625 - 634
[2] DETERMINATION OF THE RATE OF BASE-PAIR SUBSTITUTION AND INSERTION MUTATIONS IN RETROVIRUS REPLICATION
DOUGHERTY, JP
TEMIN, HM
[J]. JOURNAL OF VIROLOGY, 1988, 62 (08) : 2817 - 2822
[3] SEPARATION OF IL-4 PRODUCTION FROM TH-CELL PROLIFERATION BY AN ALTERED T-CELL RECEPTOR LIGAND
EVAVOLD, BD
ALLEN, PM
[J]. SCIENCE, 1991, 252 (5010) : 1308 - 1310
[4] TICKLING THE TCR - SELECTIVE T-CELL FUNCTIONS STIMULATED BY ALTERED PEPTIDE LIGANDS
EVAVOLD, BD
SLOANLANCASTER, J
ALLEN, PM
[J]. IMMUNOLOGY TODAY, 1993, 14 (12): : 602 - 609
[5] T-CELL RECEPTOR ANTAGONIST PEPTIDES INDUCE POSITIVE SELECTION
HOGQUIST, KA
JAMESON, SC
HEATH, WR
HOWARD, JL
BEVAN, MJ
CARBONE, FR
[J]. CELL, 1994, 76 (01) : 17 - 27
[6] CLONE-SPECIFIC T-CELL RECEPTOR ANTAGONISTS OF MAJOR HISTOCOMPATIBILITY COMPLEX CLASS-I RESTRICTED CYTOTOXIC T-CELLS
JAMESON, SC
CARBONE, FR
BEVAN, MJ
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1993, 177 (06) : 1541 - 1550
[7] MACKETT M, 1984, J VIROL, V49, P854
[8] Maniatis T., 1982, MOL CLONING
[9] MYERS G, 1992, HUMAN RETROVIRUSES A
[10] HIV-1 GAG-SPECIFIC CYTO-TOXIC LYMPHOCYTES-T DEFINED WITH RECOMBINANT VACCINIA VIRUS AND SYNTHETIC PEPTIDES
NIXON, DF
TOWNSEND, ARM
ELVIN, JG
RIZZA, CR
GALLWEY, J
MCMICHAEL, AJ
[J]. NATURE, 1988, 336 (6198) : 484 - 487

← 1 2 →