建立 Zika 病毒相关出生缺陷的非人灵长类动物模型。
Modeling Zika Virus-Associated Birth Defects in Nonhuman Primates.
机构信息
Department of Pediatrics, University of Wisconsin-Madison.
出版信息
J Pediatric Infect Dis Soc. 2018 Dec 26;7(suppl_2):S60-S66. doi: 10.1093/jpids/piy120.
Abstract
In utero infection with Zika virus (ZIKV) during pregnancy can lead to the development of birth defects and postnatal deficits. A nonhuman primate (NHP) model of congenital ZIKV infection can help fill the gaps in knowledge where tissue studies are required to define viral pathogenesis and identify targets for therapeutic intervention. This model system has already identified critical features of ZIKV pathogenesis in congenital infection. Before translating these NHP studies to human clinical trials, we must understand the similarities and differences between human and NHP fetal immune system development, neural development, and infant assessment tools. Because of the overall similarity between fetal and infant development in humans and NHPs, this NHP model can complement human clinical trials by defining immune correlates of protection and evaluating therapeutic interventions.
摘要
妊娠期间 Zika 病毒(ZIKV)宫内感染可导致出生缺陷和产后缺陷。先天性 ZIKV 感染的非人灵长类动物(NHP)模型有助于填补知识空白,这些知识需要组织研究来定义病毒发病机制和确定治疗干预的靶点。该模型系统已经确定了先天性感染中 ZIKV 发病机制的关键特征。在将这些 NHP 研究转化为人类临床试验之前,我们必须了解人类和 NHP 胎儿免疫系统发育、神经发育和婴儿评估工具之间的相似性和差异。由于人类和 NHP 胎儿和婴儿发育的总体相似性,该 NHP 模型可以通过定义保护的免疫相关性和评估治疗干预来补充人类临床试验。
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