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Disease modeling for Ebola and Marburg viruses

机译:埃博拉和马尔堡病毒的疾病模型

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The filoviruses Ebola and Marburg are zoonotic agents that are classified as both biosafety level 4 and category A list pathogens. These viruses are pathogenic in humans and cause isolated infections or epidemics of viral hemorrhagic fever, mainly in Central Africa. Their natural reservoir has not been definitely identified, but certain species of African bat have been associated with Ebola and Marburg infections. Currently, there are no licensed options available for either treatment or prophylaxis. Different animal models have been developed for filoviruses including mouse, guinea pig and nonhuman primates. The ‘gold standard’ animal models for pathogenesis, treatment and vaccine studies are rhesus and cynomolgus macaques. This article provides a brief overview of the clinical picture and the pathology/pathogenesis of human filovirus infections. The current animal model options are discussed and compared with regard to their value in different applications. In general, the small animal models, in particular the mouse, are the most feasible for high biocontainment facilities and they offer the most options for research owing to the greater availability of immunologic and genetic tools. However, their mimicry of the human diseases as well as their predictive value for therapeutic efficacy in primates is limited, thereby making them, at best, valuable initial screening tools for pathophysiology, treatment and vaccine studies.
机译:线状病毒埃博拉病毒和马尔堡病毒是人畜共患病菌,被分类为生物安全级别4和A类清单病原体。这些病毒在人类中具有致病性,并引起病毒性出血热的单独感染或流行,主要在中部非洲。它们的天然储层尚未得到明确鉴定,但是某些非洲蝙蝠物种与埃博拉和马尔堡感染有关。当前,没有许可的选项可用于治疗或预防。已开发出针对丝状病毒的不同动物模型,包括小鼠,豚鼠和非人类灵长类动物。用于发病机理,治疗和疫苗研究的“金标准”动物模型是恒河猴和食蟹猕猴。本文简要概述了人类丝状病毒感染的临床情况以及病理/发病机理。讨论并比较了当前动物模型选项在不同应用中的价值。通常,小型动物模型,尤其是小鼠,对于高生物安全设施而言是最可行的,并且由于免疫和遗传工具的可用性更高,它们为研究提供了最多的选择。但是,它们对人类疾病的模仿以及对灵长类动物治疗功效的预测价值受到限制,因此,它们充其量只能作为病理生理,治疗和疫苗研究的宝贵初始筛选工具。

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