Natural history of Sudan ebolavirus infection in rhesus and cynomolgus macaques.

IF 0.3 Q4 EDUCATION & EDUCATIONAL RESEARCH
Courtney Woolsey, Alyssa C Fears, Viktoriya Borisevich, Krystle N Agans, Natalie S Dobias, Abhishek N Prasad, Daniel J Deer, Joan B Geisbert, Karla A Fenton, Thomas W Geisbert, Robert W Cross
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Abstract

Due to its high mortality rate and continued re-emergence, Ebolavirus disease (EVD) continues to pose a serious threat to global health. A group of viruses within the genus Ebolavirus causes this severe hemorrhagic disease in humans: Ebola virus (EBOV; species Zaire ebolavirus), Sudan virus (SUDV; species Sudan ebolavirus), Bundibugyo virus, and Taï Forest virus. EBOV and SUDV are associated with the highest case fatality rates. While the host response to EBOV has been comprehensively examined, limited data exists for SUDV infection. For medical countermeasure testing, well-characterized SUDV nonhuman primate (NHP) models are thus needed. Here, we describe a natural history study in which rhesus (N = 11) and cynomolgus macaques (N = 14) were intramuscularly exposed to a 1000 plaque-forming unit dose of SUDV (Gulu variant). Time-course analyses of various hematological, pathological, serological, coagulation, and transcriptomic findings are reported. SUDV infection was uniformly lethal in cynomolgus macaques (100% mortality), whereas a single rhesus macaque subject (91% mortality) survived to the study endpoint (median time-to-death of ∼8.0 and ∼8.5 days in cynomolgus and rhesus macaques, respectively). Infected macaques exhibited hallmark features of human EVD. The early stage was typified by viremia, granulocytosis, lymphopenia, albuminemia, thrombocytopenia, and decreased expression of HLA-class transcripts. At mid-to-late disease, animals developed fever and petechial rashes, and expressed high levels of pro-inflammatory mediators, pro-thrombotic factors, and markers indicative of liver and kidney injury. End-stage disease was characterized by shock and multi-organ failure. In summary, macaques recapitulate human SUDV disease, supporting these models for use in the development of vaccines and therapeutics.

恒河猴和猕猴感染苏丹伊波拉病毒的自然史。
埃博拉病毒病(EVD)死亡率高,且不断复发,继续对全球健康构成严重威胁。埃博拉病毒属中的一组病毒会导致人类患上这种严重的出血性疾病:埃博拉病毒(EBOV;扎伊尔埃博拉病毒属)、苏丹病毒(SUDV;苏丹埃博拉病毒属)、本迪布吉病毒和塔伊森林病毒。EBOV 和 SUDV 的病死率最高。虽然宿主对 EBOV 的反应已得到全面研究,但关于 SUDV 感染的数据却很有限。因此,医疗对策测试需要特性良好的 SUDV 非人灵长类动物(NHP)模型。在本文中,我们描述了一项自然史研究,恒河猴(11 只)和犬猕猴(14 只)肌肉注射了 1000 个斑块形成单位剂量的 SUDV(古卢变种)。报告了各种血液学、病理学、血清学、凝血学和转录组学结果的时程分析。犬科猕猴感染 SUDV 后一致死亡(100% 死亡率),而只有一只猕猴(91% 死亡率)存活到研究终点(犬科猕猴和猕猴的中位死亡时间分别为 8.0 天和 8.5 天)。受感染的猕猴表现出人类EVD的特征。早期表现为病毒血症、粒细胞减少、淋巴细胞减少、白蛋白血症、血小板减少和HLA类转录物表达减少。在疾病的中晚期,动物出现发热和瘀斑皮疹,并表达高水平的促炎介质、促血栓形成因子以及表明肝脏和肾脏损伤的标志物。疾病晚期的特征是休克和多器官衰竭。总之,猕猴再现了人类 SUDV 疾病,支持将这些模型用于疫苗和疗法的开发。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Enunciacion
Enunciacion EDUCATION & EDUCATIONAL RESEARCH-
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11
审稿时长
6 weeks
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