Zhu M, Terasawa H, Gulley J, Panicali D, Arlen P, Schlom J, Tsang K Y
Laboratory of Tumor Immunology and Biology, National Cancer Institute, NIH, Bethesda, Maryland 20892-1750, USA.
Cancer Res. 2001 May 1;61(9):3725-34.
T-cell activation usually requires at least two signals. The first signal is antigen-specific, and the second signal(s) involves the interaction of a T-cell costimulatory molecule(s) on the antigen-presenting cell (APC) with its ligand on the T cell. Dendritic cells (DCs) are the most potent APCs, attributable, in part, to their expression of several T-cell costimulatory molecules. Human DCs generated in vitro, however, will vary in methods of generation and maturation and in terms of expression of different phenotypic markers-including costimulatory molecules-among different donors. We report here that a recombinant avipox (fowlpox, rF) vector has been constructed that can efficiently express the transgenes for three human T-cell costimulatory molecules (B7-1, ICAM-1, and LFA-3) as a result of individual early avipox promoters driving the expression of each transgene. This triad of costimulatory molecules (designated TRICOM) was selected because each has an individual ligand on T cells and each has been shown previously to prime a unique signaling pathway in T cells. We report here that rF-TRICOM can efficiently infect human DCs of different states of maturity and hyperexpress each of the three costimulatory molecules on the DC surface without affecting other DC phenotypic markers. Infection of influenza or human papilloma virus 9-mer peptide-pulsed DCs from different individuals, or at different stages of maturity with rF-TRICOM, resulted in enhanced activation of T cells from peripheral blood mononuclear cells of autologous donors after 24 h of incubation with DCS: This enhanced activation was analyzed by both titrating the peptide and differing the DC:effector cell ratios. No effect was observed using the control wild-type avipox vector. No increase in apoptosis was observed in T cells hyperstimulated with the TRICOM vector, and no decrease in interleukin-12 production was seen in lipopolysaccharide-stimulated DCs infected with rF-TRICOM. Antibody-blocking experiments demonstrated that enhanced T-cell activation by TRICOM was attributed to each of the three costimulatory molecules. Peptide-pulsed, rF-TRICOM-infected DCs were also shown to be more effective than peptide-pulsed DCs in activating T cells to 9-mer peptides derived from two relatively weak "self" immunogens, i.e., human prostate-specific antigen and human carcinoembryonic antigen. These studies thus demonstrate for the first time that a vector that can simultaneously hyperexpress three costimulatory molecules can be used to efficiently infect human DCs, leading to enhanced peptide-specific T-cell activation. The use of this approach for in vitro studies and clinical applications in immunotherapy is discussed.
T细胞活化通常至少需要两个信号。第一个信号是抗原特异性的,第二个信号涉及抗原呈递细胞(APC)上的T细胞共刺激分子与其在T细胞上的配体之间的相互作用。树突状细胞(DC)是最有效的APC,部分原因在于它们表达多种T细胞共刺激分子。然而,体外产生的人DC在产生和成熟方法以及不同供体之间在不同表型标志物(包括共刺激分子)的表达方面会有所不同。我们在此报告,已构建了一种重组禽痘病毒(鸡痘病毒,rF)载体,由于单个早期禽痘病毒启动子驱动每个转基因的表达,该载体可有效表达三种人T细胞共刺激分子(B7-1、ICAM-1和LFA-3)的转基因。选择这三种共刺激分子的组合(称为TRICOM)是因为它们在T细胞上各自具有配体,并且先前已证明它们各自在T细胞中引发独特的信号通路。我们在此报告,rF-TRICOM可以有效感染不同成熟状态的人DC,并在DC表面超表达这三种共刺激分子中的每一种,而不影响其他DC表型标志物。用rF-TRICOM感染来自不同个体或处于不同成熟阶段的流感或人乳头瘤病毒9聚体肽脉冲DC,在与DC孵育24小时后,导致来自自体供体外周血单核细胞的T细胞活化增强:通过滴定肽和改变DC与效应细胞比例来分析这种增强的活化。使用对照野生型禽痘病毒载体未观察到效果。用TRICOM载体过度刺激的T细胞中未观察到凋亡增加,用rF-TRICOM感染的脂多糖刺激的DC中白细胞介素-12的产生也未减少。抗体阻断实验表明,TRICOM增强的T细胞活化归因于这三种共刺激分子中的每一种。肽脉冲、rF-TRICOM感染的DC在激活T细胞对源自两种相对较弱的“自身”免疫原(即人前列腺特异性抗原和人癌胚抗原)的9聚体肽方面也比肽脉冲DC更有效。因此,这些研究首次证明,一种能够同时超表达三种共刺激分子的载体可用于有效感染人DC,从而增强肽特异性T细胞活化。讨论了这种方法在体外研究和免疫治疗临床应用中的用途。
