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CYTOTOXIC T-LYMPHOCYTE RESPONSES TO THE ENVELOPE PROTEINS OF ENDOGENOUS ECOTROPIC AND MINK CYTOPATHIC FOCUS-FORMING MURINE LEUKEMIA VIRUSES IN H-2(B) MICE

被引:19
作者
COPPOLA, MA [1 ]
GREEN, WR [1 ]
机构
[1] DARTMOUTH COLL SCH MED,NORRIS COTTON CANC CTR,LEBANON,NH 03756
来源
VIROLOGY | 1994年 / 202卷 / 01期
关键词
D O I
10.1006/viro.1994.1370
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
To study the possible role of immune selection in the in vivo generation of pathogenic recombinant murine leukemia viruses (MuLV), we have constructed recombinant vaccinia viruses (rVV) expressing the envelope genes of three MuLV: AKR623, MCF247, and MCF13. rVV expressing either AKR623 or MCF247 env could prime H-2(b) mice for anti-AKR/Gross virus CTL responses, and stimulate the in vitro generation of CTL from the spleens of mice immunized with an AKR/Gross virus-positive lymphoma. MC57 (H-2(b)) cells infected with either 623EnvVac or 247EnvVac could serve as targets for AKR/ Gross virus-specific CTL. Cells infected with the rVV expressing MCF13 env, however, were lysed much less efficiently by these CTL. 13EnvVac was also ineffective in priming or stimulating retrovirus-specific CTL. Finally, experiments with synthetic peptides and minigenes suggested that the reduced immunogenicity of the MCF13 envelope protein likely resulted from a single amino acid substitution within an immunodominant epitope of the p15E (TM) protein. The region of MCF13 env that encodes this epitope is derived from an endogenous xenotropic virus, while the allelic sequences in MCF247 are of ecotropic virus origin. These results suggest the potential for recombination within the MuLV envelope gene to allow escape from host cellular immune responses. (C) 1994 Academic Press, Inc
引用
收藏
页码:500 / 505
页数:6
相关论文
共 38 条
[1]   ORIGIN OF MINK CYTOPATHIC FOCUS-FORMING (MCF) VIRUSES - COMPARISON WITH ECOTROPIC AND XENOTROPIC MURINE LEUKEMIA-VIRUS GENOMES [J].
CHATTOPADHYAY, SK ;
LANDER, MR ;
GUPTA, S ;
RANDS, E ;
LOWY, DR .
VIROLOGY, 1981, 113 (02) :465-483
[2]   CELLULAR-ORIGIN AND ROLE OF MINK CELL FOCUS-FORMING VIRUSES IN MURINE THYMIC LYMPHOMAS [J].
CHATTOPADHYAY, SK ;
CLOYD, MW ;
LINEMEYER, DL ;
LANDER, MR ;
RANDS, E ;
LOWY, DR .
NATURE, 1982, 295 (5844) :25-31
[3]   CHARACTERIZATION OF MOUSE MONOCLONAL-ANTIBODIES SPECIFIC FOR FRIEND MURINE LEUKEMIA VIRUS-INDUCED ERYTHROLEUKEMIA-CELLS - FRIEND-SPECIFIC AND FMR-SPECIFIC ANTIGENS [J].
CHESEBRO, B ;
WEHRLY, K ;
CLOYD, M ;
BRITT, W ;
PORTIS, J ;
COLLINS, J ;
NISHIO, J .
VIROLOGY, 1981, 112 (01) :131-144
[4]   A HOST GENE REGULATES THE STRUCTURE OF THE TRANSMEMBRANE ENVELOPE PROTEIN OF MURINE LEUKEMIA VIRUSES [J].
COPPOLA, MA ;
THOMAS, CY .
JOURNAL OF EXPERIMENTAL MEDICINE, 1990, 171 (05) :1739-1752
[5]  
EARL P, 1990, J VIROL, V65, P31
[6]  
EARL PL, 1993, CURRENT PROTOCOLS MO
[7]   EXPRESSION OF A MEMBRANE PROTEASE ENHANCES PRESENTATION OF ENDOGENOUS ANTIGENS TO MHC CLASS I-RESTRICTED LYMPHOCYTES-T [J].
EISENLOHR, LC ;
BACIK, I ;
BENNINK, JR ;
BERNSTEIN, K ;
YEWDELL, JW .
CELL, 1992, 71 (06) :963-972
[8]   BIOCHEMICAL EVIDENCE THAT MCF MURINE LEUKEMIA VIRUSES ARE ENVELOPE (ENV) GENE RECOMBINANTS [J].
ELDER, JH ;
GAUTSCH, JW ;
JENSEN, FC ;
LERNER, RA ;
HARTLEY, JW ;
ROWE, WP .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1977, 74 (10) :4676-4680
[9]   FRIEND AND MOLONEY MURINE LEUKEMIA VIRUSES SPECIFICALLY RECOMBINE WITH DIFFERENT ENDOGENOUS RETROVIRAL SEQUENCES TO GENERATE MINK CELL FOCUS-FORMING VIRUSES [J].
EVANS, LH ;
CLOYD, MW .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1985, 82 (02) :459-463
[10]   ALLELE-SPECIFIC MOTIFS REVEALED BY SEQUENCING OF SELF-PEPTIDES ELUTED FROM MHC MOLECULES [J].
FALK, K ;
ROTZSCHKE, O ;
STEVANOVIC, S ;
JUNG, G ;
RAMMENSEE, HG .
NATURE, 1991, 351 (6324) :290-296
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