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Differential Neurovirulence of African and Asian Genotype Zika Virus Isolates in Outbred Immunocompetent Mice

机译:非洲和亚洲基因型Zika病毒中差异神经潜伏在近期免疫活性小鼠中的病毒

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Although first isolated almost 70 years ago, Zika virus (ZIKV; Flavivirus, Flaviviridae) has only recently been associated with significant outbreaks of disease in humans. Several severe ZIKV disease manifestations have also been recently documented, including fetal malformations, such as microcephaly, and Guillain-Barre syndrome in adults. Although principally transmitted by mosquitoes, sexual transmission of ZIKV has been documented. Recent publications of several interferon receptor knockout mouse models have demonstrated ZIKV-induced disease. Herein, outbred immunocompetent CD-1/ICR adult mice were assessed for susceptibility to disease by intracranial (i.c.) and intraperitoneal (i.p.) inoculation with the Ugandan prototype strain (MR766; African genotype), a low-passage Senegalese strain (DakAr41524; African genotype) and a recent ZIKV strain isolated from a traveler infected in Puerto Rico (PRVABC59; Asian genotype). Morbidity was not observed in mice inoculated by the i.p. route with either MR766 or PRVABC59 for doses up to 6 log(10) PFU. In contrast, CD-1/ICR mice inoculated i.c. with the MR766 ZIKV strain exhibited an 80-100% mortality rate that was age independent. The DakAr41524 strain delivered by the i.c route caused 30% mortality, and the Puerto Rican ZIKV strain failed to elicit mortality but did induce a serum neutralizing immune response in 60% of mice. These data provide a potential animal model for assessing neurovirulence determinants of different ZIKV strains as well as a potential immunocompetent challenge model for assessing protective efficacy of vaccine candidates.
机译:虽然近70年前的首次孤立,但Zika病毒(Zikv; Flavivirus,Flaviviridae)最近才与人类的重大爆发有关。最近还记录了几种严重的ZIKV病表现,包括胎儿畸形,如微微症和成年人的Guillain-Barre综合征。虽然主要由蚊子传播,但ZIKV的性传播已被记录。最近几种干扰素受体敲除小鼠模型的出版物表现出ZIKV诱导的疾病。在此,通过颅内(IC)和腹膜内(IP)与乌干达原型菌株(MR766;非洲基因型)接种,评估对疾病的敏感性的差异免疫紊乱CD-1 / ICR成年小鼠,低通塞内加尔菌株(Dakar41524;非洲人基因型)和最近从波多黎各感染的旅行者孤立的ZIKV菌株(PRVABC59;亚洲基因型)。在I.P的小鼠中未观察到发病率。用于MR766或PRVABC59的用于剂量,最多可用6个log(10)pfu。相比之下,CD-1 / ICR小鼠接种I.C。随着MR766的ZIKV菌株表现出80-100%的死亡率,年龄独立。由I.C路线提供的Dakar41524菌株引起了30%的死亡率,波多黎各ZIKV菌株未能引发死亡率,但在60%的小鼠中诱导血清中和免疫应答。这些数据提供了用于评估不同ZIKV菌株的神经血管血管决定簇的潜在动物模型以及用于评估疫苗候选物的保护效果的潜在免疫活性挑战模型。

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