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A Comparison of the Pathogenesis of Marburg Virus Disease in Humans and Nonhuman Primates and Evaluation of the Suitability of These Animal Models for Predicting Clinical Efficacy under the 'Animal Rule'

机译:人类和非人类灵长类动物马尔堡病毒病发病机制的比较以及“动物规则”下这些动物模型对临床疗效预测的适用性评估

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摘要

Marburg virus outbreaks are sporadic, infrequent, brief, and relatively small in terms of numbers of subjects affected. In addition, outbreaks most likely will occur in remote regions where clinical trials are not feasible; therefore, definitive, well-controlled human efficacy studies to test the effectiveness of a drug or biologic product are not feasible. Healthy human volunteers cannot ethically be deliberately exposed to a lethal agent such as Marburg virus in order to test the efficacy of a therapy or preventive prior to licensure. When human efficacy studies are neither ethical nor feasible, the US Food and Drug Administration may grant marketing approval of a drug or biologic product under the 'Animal Rule,' through which demonstration of the efficacy of a product can be 'based on adequate and well-controlled animal efficacy studies when the results of those studies establish that the drug is reasonably likely to produce clinical benefit in humans.' This process requires that the pathogenic determinants of the disease in the animal model are similar to those that have been identified in humans. After reviewing primarily English-language, peer-reviewed journal articles, we here summarize the clinical manifestations of Marburg virus disease and the results of studies in NHP showing the characteristics and progression of the disease. We also include a detailed comparison of the characteristics of the human disease relative to those for NHP. This review reveals that the disease characteristics of Marburg virus disease are generally similar for humans and 3 NHP species: cynomolgus macaques (Macaca fascicularis), rhesus macaques (Macaca mulatta), and African green monkeys (Chlorocebus aethiops).
机译:马尔堡病毒的爆发是偶发的,不频繁的,短暂的,并且就受感染的对象而言而言相对较小。此外,暴发很可能发生在临床试验不可行的偏远地区。因此,进行明确,控制良好的人类功效研究以测试药物或生物制品的有效性是不可行的。健康的人类志愿者不能从伦理上有意地暴露于致死剂(如马尔堡病毒)中,以在获得许可之前测试疗法或预防剂的功效。当人类功效研究既不道德也不可行时,美国食品和药物管理局可能会根据“动物法则”授予药品或生物制品的市场批准,通过该法则可以“充分且充分地”证明产品功效对照的动物功效研究,当这些研究的结果确定该药物合理地可能对人类产生临床益处时。”该过程要求动物模型中疾病的致病因素与在人类中确定的那些因素相似。在主要回顾了英语,同行评审的期刊文章之后,我们在这里总结了马尔堡病毒病的临床表现以及在NHP中显示疾病特征和进展的研究结果。我们还包括相对于NHP的人类疾病特征的详细比较。这项审查表明,人类和3种NHP物种的马尔堡病毒病的疾病特征通常相似:食蟹猕猴(Macaca fascicularis),恒河猴(Macaca mulatta)和非洲绿猴(Chlorocebus aethiops)。

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