Proteasome-independent major histocompatibility complex class I cross-presentation mediated by papaya mosaic virus-like particles leads to expansion of specific human T cells

被引:56
作者
Leclerc, Denis
Beauseigle, Diane
Denis, Jerome
Morin, Helene
Pare, Christine
Lamarre, Alain
Lapointe, Rejean
机构
[1] Univ Montreal, Hop Notre Dame de Bon Secours, CHUM, Ctr Rech, Montreal, PQ H2L 4M1, Canada
[2] Univ Laval, Ctr Rech Infectiol, CHUL, Lauriel, PQ, Canada
[3] INRS, Inst Armand Frappier, Laval, PQ, Canada
关键词
D O I
10.1128/JVI.01720-06
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
The development of versatile vaccine platforms is a priority that is recognized by health authorities worldwide; such platforms should induce both arms of the immune system, the Immoral and cytotoxic-Tlymphocyte responses. In this study, we have established that a vaccine platform based on the coat protein of papaya mosaic virus (PapW CP), previously shown to induce a humoral response, can induce major histocompatibility complex (MHC) class I cross-presentation of HLA-A*0201 epitopes from gp100, a melanoma antigen, and from influenza virus M1 matrix protein. PapW proteins were able to assemble into stable virus-like particles (VLPs) in a crystalline and repetitive structure. When we pulsed HIA-A*0201(+) antigen-presenting cells (APCs) with the recombinant PapW FLU or gp100, we noted that antigen-specific CD8(+) T cells were highly reactive to these APCs, demonstrating that the epitope from the VLPs were processed and loaded on the MHC class I complex. APCs were preincubated with two different proteasome inhibitors, which did not affect the efficiency of peptide presentation on MHC class I. Classical presentation from an endogenous antigen was abolished in the same conditions. Clearly, antigen presentation mediated by the PapMV system was proteasome independent. Finally, PapW-pulsed APCs had the capacity to expand highly avid antigen-specific T cells against the influenza virus M1 HLA-A*0201 epitope when cocultured with autologous peripheral blood mononuclear cells. This study demonstrates the potential of PapMV for MHC class I cross-presentation and for the expansion of human antigen-specific T cells. It makes VLPs from PapMV CP a very attractive platform to trigger cellular responses for vaccine development against chronic infectious diseases and cancers.
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页码:1319 / 1326
页数:8
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