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首页> 外文期刊>Cancer research: The official organ of the American Association for Cancer Research, Inc >Paradoxical Decrease in the Capture and Lymph Node Delivery of Cancer Vaccine Antigen Induced by a TLR4 Agonist as Visualized by Dual-Mode Imaging
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Paradoxical Decrease in the Capture and Lymph Node Delivery of Cancer Vaccine Antigen Induced by a TLR4 Agonist as Visualized by Dual-Mode Imaging

机译:由双模式成像可视化由TLR4激动剂诱导的癌症疫苗抗原的捕获和淋巴结传递中的自相矛盾的减少。

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摘要

Traditionally, cell-mediated immune responses to vaccination in animal models are evaluated by invasive techniques such as biopsy and organ extraction. We show here that by combining two noninvasive imaging technologies, MRI and bioluminescence imaging (BLI), we can visualize both the afferent and efferent arms of cellular events following vaccination longitudinally. To this end, we evaluated the immune response elicited by a novel Toll-like receptor 4 agonist vaccine adjuvant, glucopyranosyl lipid A (GLA), using a whole-cell tumor vaccine. After magnetovaccination, MRI was used to visualize antigen-presenting cell-mediated antigen capture and subsequent migration to draining lymph nodes (DLN). Paradoxically, we observed that the incorporation of GLA in the vaccine reduced these critical parameters of the afferent immune response. For the efferent arm, the magnitude of the ensuing antigen-specific T-cell response in DLN visualized using BLI correlated with antigen delivery to the DLN as measured by MRI. These findings were confirmed using flow cytometry. In spite of the GLA-associated reduction in antigen delivery to the DLN, however, the use of GLA as a vaccine adjuvant led to a massive proliferation of vaccine primed antigen-specific T cells in the spleen. This was accompanied by an enhanced tumor therapeutic effect of the vaccine. These findings suggest that GLA adjuvant changes the temporal and anatomical features of both the afferent and efferent arms of the vaccine response and illustrates the utility of quantitative noninvasive imaging as a tool for evaluating these parameters during vaccine optimization. (C)2014 AACR.
机译:传统上,在动物模型中细胞介导的对疫苗接种的免疫反应是通过侵入性技术(如活检和器官提取)进行评估的。我们在这里展示了通过结合MRI和生物发光成像(BLI)这两种非侵入性成像技术,我们可以在纵向接种疫苗后可视化细胞事件的传入和传出臂。为此,我们使用全细胞肿瘤疫苗评估了由新型Toll样受体4激动剂疫苗佐剂吡喃葡萄糖基脂质A(GLA)引发的免疫反应。磁化卵泡接种后,MRI用于可视化抗原呈递细胞介导的抗原捕获以及随后迁移至引流淋巴结(DLN)的过程。矛盾的是,我们观察到疫苗中加入GLA降低了传入免疫反应的这些关键参数。对于传出臂,使用MRI观察到的DLN中随后发生的抗原特异性T细胞反应的强度与通过MRI测量的向DLN的抗原传递相关。使用流式细胞仪证实了这些发现。然而,尽管与GLA相关的向DLN的抗原递送减少,但是使用GLA作为疫苗佐剂导致疫苗引发的脾脏中抗原特异性T细胞的大量增殖。这伴随着疫苗的增强的肿瘤治疗作用。这些发现表明,GLA佐剂改变了疫苗反应传入和传出臂的时间和解剖特征,并说明了定量无创成像作为评估疫苗优化过程中这些参数的工具的实用性。 (C)2014 AACR。

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