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Induction of T-cell memory by a dendritic cell vaccine: a computational model

机译:树突状细胞疫苗诱导T细胞记忆的计算模型

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Motivation: Although results from phase III clinical trials substantially support the use of prophylactic and therapeutic vaccines against cancer, what has yet to be defined is how many and how frequent boosts are needed to sustain a long-lasting and protecting memory T-cell response against tumor antigens. Common experience is that such preclinical tests require the sacrifice of a relatively large number of animals, and are particularly time-and money-consuming. Results: As a first step to overcome these hurdles, we have developed an ordinary differential equation model that includes all relevant entities (such as activated cytotoxic T lymphocytes and memory T cells), and investigated the induction of immunological memory in the context of wild-type mice injected with a dendritic cell-based vaccine. We have simulated the biological behavior both in the presence and in the absence of memory T cells. Comparing results of ex vivo and in silico experiments, we show that the model is able to envisage the expansion and persistence of antigen-specific memory T cells. The model might be applicable to more complex vaccination schedules and substantially in any biological condition of prime-boosting. Availability and implementation: The model is fully described in the article
机译:动机:尽管III期临床试验的结果在很大程度上支持了针对癌症的预防性和治疗性疫苗的使用,但尚需确定需要多少剂量和频率的增强才能维持持久的和保护性的记忆性T细胞应答以抵抗肿瘤抗原。共同的经验是,这种临床前测试需要牺牲相对大量的动物,并且特别耗时和耗钱。结果:作为克服这些障碍的第一步,我们开发了一个包含所有相关实体(例如活化的细胞毒性T淋巴细胞和记忆T细胞)的普通微分方程模型,并研究了在野生环境下诱导免疫记忆的过程。注射了树突状细胞疫苗的2型小鼠。我们已经模拟了存在和不存在记忆T细胞的生物学行为。比较离体实验和计算机模拟实验的结果,我们表明该模型能够设想抗原特异性记忆T细胞的扩增和持久性。该模型可能适用于更复杂的疫苗接种时间表,并且基本上可以在任何生物学上提高免疫力的条件下使用。可用性和实现:该模型在本文中有完整描述

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