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The use of mice lacking type I or both type I and type II interferon responses in research on hemorrhagic fever viruses. Part 2: Vaccine efficacy studies

机译:在出血热病毒研究中使用缺乏I型或I型和II型干扰素反应的小鼠。 第2部分:疫苗疗效研究

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For more than 20 years, researchers have used laboratory mice lacking type I or both type I and II interferon (IFN) responses to study high-containment viruses that cause hemorrhagic fevers (HF) in humans. With the exception of Rift Valley fever virus, agents that cause viral HF in humans, such as Ebola and Lassa virus, do not cause disease in mature immunocompetent mice. In contrast, IFN-deficient mice typically develop severe or fatal disease when inoculated with these agents. The sensitivity of IFN-deficient mice to disease has led to their widespread use in biocontainment laboratories to assess the efficacy of novel vaccines against HF viruses, often without considering whether adaptive immune responses in IFN-deficient mice accurately mirror those in immunocompetent humans. Failure to recognize these questions may lead to inappropriate expectations of the predictive value of mouse experiments. In two invited articles, we investigate these questions. The present article reviews the use of IFN-deficient mice for assessing novel vaccines against HF viruses, including Ebola, Lassa, Crimean-Congo hemorrhagic fever and Rift Valley fever viruses. A companion paper examines the general question of how the lack of IFN signaling may affect adaptive immune responses and the outcome of vaccine studies in mice.
机译:20多年以上,研究人员使用缺乏I型或I型和II型干扰素(IFN)反应的实验室小鼠研究人类中引起出血性烧伤(HF)的高含量病毒。除了裂谷发热病毒外,导致人类病毒HF的药剂,例如埃博拉和兰萨病毒,不会引起成熟免疫活性小鼠的疾病。相反,IFN缺陷小鼠通常在接种与这些药剂接种时产生严重或致命的疾病。 IFN缺乏小鼠对疾病的敏感性导致了它们在生物土壤实验室中广泛使用,以评估新疫苗对HF病毒的疗效,而不是考虑到IFN缺陷小鼠中的适应性免疫反应是否准确地镜像免疫活性人体中的那些。未能认识到这些问题可能导致小鼠实验预测值的不恰当期望。在两个邀请的文章中,我们调查了这些问题。本文审查了IFN缺陷的小鼠用于评估针对HF病毒的新型疫苗,包括埃博拉,兰萨,克里米亚 - 刚果出血热和裂谷发热病毒。伴侣纸张审查了如何缺乏IFN信号传导的一般问题可能影响自适应免疫应答以及小鼠疫苗研究的结果。

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