INDUCTION OF HIV-SPECIFIC CYTOTOXIC-T LYMPHOCYTES IN-VIVO WITH HYBRID HIV-1 V3-TY-VIRUS-LIKE PARTICLES

被引:0
|
作者
LAYTON, GT [1 ]
HARRIS, SJ [1 ]
GEARING, AJH [1 ]
HILLPERKINS, M [1 ]
COLE, JS [1 ]
GRIFFITHS, JC [1 ]
BURNS, NR [1 ]
KINGSMAN, AJ [1 ]
ADAMS, SE [1 ]
机构
[1] UNIV OXFORD, DEPT BIOCHEM, OXFORD OX1 3QU, ENGLAND
来源
JOURNAL OF IMMUNOLOGY | 1993年 / 151卷 / 02期
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中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
In general, it has proven difficult to induce CTL responses using simple proteins or peptides without resorting to specialized adjuvants. In this study we show that particulate polymeric Ag in the form of hybrid Ty virus-like particles carrying the V3 region of HIV-1 gp120/160 envelope protein (V3:Ty-VLP) induce V3-specific CTL in BALB/c mice in the absence of adjuvant or lipid vehicle. In vitro restimulation of splenocytes with V3 peptide was necessary in order to generate effector CTL. Th cell activation was not required for this in vitro restimulation phase. The CTL induced by the V3:Ty-VLP were CD8+ve, H-2d-restricted, and HIV-1 isolate-specific (IIIB or MN). Co-administration of IIIB V3:Ty-VLP and MN V3:Ty-VLP primed both IIIB and MN V3-specific CTL. However, only IIIB V3-specific CTL were primed by hybrid Ty-VLP carrying IIIB, MN, and RF V3 loop sequences on the same particle indicating that there is intra- but not intermolecular competition between CTL epitopes. In direct comparisons, V3:Ty-VLP were substantially more potent than rgp120. Rgp160 and a 40mer IIIB V3 peptide both failed to prime V3-specific CTL. These data suggest that the particulate nature of hybrid Ty-VLP facilitates uptake into APC with subsequent access to the MHC class I processing pathway and that they may be useful vaccine vehicles for inducing cytolytic immunity against HIV-1 and other intracellular pathogens.
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页码:1097 / 1107
页数:11
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