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Primary human T-cell responses to the major outer membrane protein of Chlamydia trachomatis.

机译:主要人类T细胞对沙眼衣原体主要外膜蛋白的反应。

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摘要

The major outer membrane protein (MOMP) of Chlamydia trachomatis is the main candidate antigen for a synthetic vaccine against chlamydial infection. Antibodies to surface-exposed epitopes on MOMP neutralize chlamydial infectivity but little is known about T-cell recognition of the molecule. We have measured primary human T-cell responses to recombinant fragments of MOMP as well as to the whole organism and synthetic MOMP peptides. Using antigen-pulsed low density cells (LDC) we were able to stimulate proliferative responses with T cells from most naive individuals. This response was antigen dose dependent and displayed an absolute requirement for dendritic cells in the antigen-presenting cell (APC) population. Several T-cell epitopes were identified in MOMP and one which stimulated T cells from 80% of donors was resolved as a 12 amino acid synthetic peptide. Dual cell surface labelling and cell cycle analysis by FACS revealed that both CD4+ and CD8+ T cells were stimulated in these cultures. The fact that we were able to obtain proliferative responses and interferon-gamma (IFN-gamma) production to MOMP using cells from cord bloods confirmed that these are genuine primary responses. These experiments have identified a region on MOMP, to which T cells from most humans make a primary response, which may be useful in a chlamydial vaccine. The approach is useful for vaccine development in general.
机译:沙眼衣原体的主要外膜蛋白(MOMP)是合成的抗衣原体感染疫苗的主要候选抗原。 MOMP表面暴露的抗原决定簇的抗体可中和衣原体感染性,但对该分子的T细胞识别知之甚少。我们已经测量了原代人T细胞对MOMP重组片段以及整个生物体和合成MOMP肽的反应。使用抗原脉冲低密度细胞(LDC),我们能够刺激来自大多数幼稚个体的T细胞的增殖反应。该反应是抗原剂量依赖性的,并且显示了对抗原呈递细胞(APC)群体中树突状细胞的绝对要求。在MOMP中鉴定出了几种T细胞表位,其中一个从80%供体中刺激T细胞的表位被解析为12个氨基酸的合成肽。通过FACS进行的双细胞表面标记和细胞周期分析表明,在这些培养物中,CD4 +和CD8 + T细胞均受到刺激。我们能够使用脐带血细胞获得对MOMP的增殖反应和干扰素-γ(IFN-γ)产生的事实,证实了这些都是真正的主要反应。这些实验已经确定了MOMP上的区域,大多数人的T细胞对该区域进行了初步反应,这可能在衣原体疫苗中有用。该方法通常可用于疫苗开发。

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