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西尼罗河/登革嵌合病毒对西尼罗河和登革热蚊媒的感染性。

Infectivity of West Nile/dengue chimeric viruses for West Nile and dengue mosquito vectors.

作者信息

Hanley Kathryn A, Goddard Laura B, Gilmore Lara E, Scott Thomas W, Speicher James, Murphy Brian R, Pletnev Alexander G

机构信息

Laboratory of Infectious Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

Vector Borne Zoonotic Dis. 2005 Spring;5(1):1-10. doi: 10.1089/vbz.2005.5.1.

Abstract

West Nile virus (WN), an agent of significant human and veterinary disease, is endemic in the Old World and rapidly spreading throughout the Americas. Vaccines are needed to halt the geographic expansion of this virus and prevent disease where it is established. However, to preclude introduction of a vaccine virus into the environment, a live attenuated WN vaccine should have low potential for transmission by mosquitoes. A chimeric WN vaccine candidate was previously generated by replacing the membrane and envelope structural protein genes of recombinant dengue type 4 virus (rDEN4) with those of WN; a derivative of this virus, WN/DEN4-3'delta30, contains a 30-nucleotide deletion in the 3' untranslated region. To assess the potential for transmission by mosquitoes of these vaccine candidates, the ability of each chimeric virus to infect the mosquito midgut, disseminate to the head, and pass into the saliva was compared to that of their wild-type parental WN and DEN4 viruses in three vector species. The WN/DEN4 chimeric viruses were significantly attenuated in both Culex tarsalis, a vector able to transmit WN but not dengue, and in Ae. aegypti, a vector able to transmit dengue but not WN. However, the chimeric viruses were as infectious as either wild-type virus for Ae. albopictus, a vector able to transmit both dengue and WN. These results indicate that chimerization caused a contraction in vector host range rather than universal attenuation for mosquitoes per se. This restriction in potential vectors renders it less likely that WN/DEN4 and WN/DEN4-3'delta30 would be transmitted from vaccinees to mosquitoes.

摘要

西尼罗河病毒(WN)是一种可引发严重人类和兽医疾病的病原体,在旧世界为地方性流行,且正在迅速蔓延至整个美洲。需要疫苗来阻止该病毒的地理扩散,并在其已传播地区预防疾病。然而,为避免疫苗病毒进入环境,减毒活WN疫苗应具有较低的经蚊子传播的可能性。先前通过用WN的膜蛋白和包膜结构蛋白基因替换重组4型登革病毒(rDEN4)的相应基因,构建了一种嵌合WN疫苗候选株;该病毒的一个衍生物WN/DEN4-3'delta30在3'非翻译区有一个30个核苷酸的缺失。为评估这些疫苗候选株经蚊子传播的可能性,在三种病媒物种中,将每种嵌合病毒感染蚊子中肠、扩散至头部并进入唾液的能力与其野生型亲本WN和DEN4病毒进行了比较。WN/DEN4嵌合病毒在能够传播WN但不能传播登革热的病媒物种致倦库蚊以及能够传播登革热但不能传播WN的埃及伊蚊中均显著减毒。然而,对于能够传播登革热和WN的白纹伊蚊而言,嵌合病毒与任一野生型病毒的传染性相当。这些结果表明,嵌合作用导致了病媒宿主范围的缩小,而非对蚊子本身的普遍减毒。潜在病媒的这种限制使得WN/DEN4和WN/DEN4-3'delta30从接种疫苗者传播给蚊子的可能性降低。

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