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两种新一代裂谷热疫苗的比较疗效

Comparative efficacy of two next-generation Rift Valley fever vaccines.

作者信息

Kortekaas J, Oreshkova N, van Keulen L, Kant J, Bosch B J, Bouloy M, Moulin V, Goovaerts D, Moormann R J M

机构信息

Department of Virology, Central Veterinary Institute of Wageningen University and Research Centre (CVI-WUR), P. O. Box 65, 8200 AB Lelystad, The Netherlands.

Department of Virology, Central Veterinary Institute of Wageningen University and Research Centre (CVI-WUR), P. O. Box 65, 8200 AB Lelystad, The Netherlands; Department of Infectious Diseases and Immunology, Virology Division, Faculty of Veterinary Medicine, Utrecht University, Yalelaan 1, 3584 CL, Utrecht, The Netherlands.

出版信息

Vaccine. 2014 Sep 3;32(39):4901-8. doi: 10.1016/j.vaccine.2014.07.037. Epub 2014 Jul 19.

Abstract

Rift Valley fever virus (RVFV) is a re-emerging zoonotic bunyavirus of the genus Phlebovirus. A natural isolate containing a large attenuating deletion in the small (S) genome segment previously yielded a highly effective vaccine virus, named Clone 13. The deletion in the S segment abrogates expression of the NSs protein, which is the major virulence factor of the virus. To develop a vaccine of even higher safety, a virus named R566 was created by natural laboratory reassortment. The R566 virus combines the S segment of the Clone 13 virus with additional attenuating mutations on the other two genome segments M and L, derived from the previously created MP-12 vaccine virus. To achieve the same objective, a nonspreading RVFV (NSR-Gn) was created by reverse-genetics, which not only lacks the NSs gene but also the complete M genome segment. We have now compared the vaccine efficacies of these two next-generation vaccines and included the Clone 13 vaccine as a control for optimal efficacy. Groups of eight lambs were vaccinated once and challenged three weeks later. All mock-vaccinated lambs developed high fever and viremia and three lambs did not survive the infection. As expected, lambs vaccinated with Clone 13 were protected from viremia and clinical signs. Two lambs vaccinated with R566 developed mild fever after challenge infection, which was associated with low levels of viral RNA in the blood, whereas vaccination with the NSR-Gn vaccine completely prevented viremia and clinical signs.

摘要

裂谷热病毒(RVFV)是一种重新出现的属于白蛉病毒属的人畜共患布尼亚病毒。一种在小(S)基因组片段中含有大的减毒缺失的天然分离株此前产生了一种高效疫苗病毒,名为克隆13。S片段中的缺失消除了NSs蛋白的表达,而NSs蛋白是该病毒的主要毒力因子。为了开发一种安全性更高的疫苗,通过天然实验室重配产生了一种名为R566的病毒。R566病毒将克隆13病毒的S片段与另外两个基因组片段M和L上的额外减毒突变相结合,这两个片段源自先前产生的MP - 12疫苗病毒。为了实现相同的目标,通过反向遗传学产生了一种非传播性RVFV(NSR - Gn),它不仅缺乏NSs基因,还缺乏完整的M基因组片段。我们现在比较了这两种下一代疫苗的疫苗效力,并将克隆13疫苗作为最佳效力的对照。将八只羔羊分为一组,接种一次疫苗,三周后进行攻毒。所有 mock - 接种的羔羊都出现了高烧和病毒血症,三只羔羊在感染中没有存活下来。正如预期的那样,接种克隆13疫苗的羔羊免受了病毒血症和临床症状的影响。接种R566疫苗的两只羔羊在攻毒感染后出现了轻度发热,这与血液中低水平的病毒RNA有关,而接种NSR - Gn疫苗则完全预防了病毒血症和临床症状。

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