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Concurrent micro-RNA mediated silencing of tick-borne flavivirus replication in tick vector and in the brain of vertebrate host

机译:tick虫载体和脊椎动物宿主脑中tick传黄病毒复制的同时微RNA介导沉默。

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Tick-borne viruses include medically important zoonotic pathogens that can cause life-threatening diseases. Unlike mosquito-borne viruses, whose impact can be restrained via mosquito population control programs, for tick-borne viruses only vaccination remains the reliable means of disease prevention. For live vaccine viruses a concern exists, that spillovers from viremic vaccinees could result in introduction of genetically modified viruses into sustainable tick-vertebrate host transmission cycle in nature. To restrict tick-borne flavivirus (Langat virus, LGTV) vector tropism, we inserted target sequences for tick-specific microRNAs (mir-1, mir-275 and mir-279) individually or in combination into several distant regions of LGTV genome. This caused selective attenuation of viral replication in tick-derived cells. LGTV expressing combinations of target sequences for tick- and vertebrate CNS-specific miRNAs were developed. The resulting viruses replicated efficiently and remained stable in simian Vero cells, which do not express these miRNAs, however were severely restricted to replicate in tick-derived cells. In addition, simultaneous dual miRNA targeting led to silencing of virus replication in live Ixodes ricinus ticks and abolished virus neurotropism in highly permissive newborn mice. The concurrent restriction of adverse replication events in vertebrate and invertebrate hosts will, therefore, ensure the environmental safety of live tick-borne virus vaccine candidates.
机译:ick传播的病毒包括医学上重要的人畜共患病原体,它们可能导致威胁生命的疾病。与蚊媒病毒不同,蚊媒病毒的影响可以通过蚊子种群控制计划来限制,而tick虱病毒仅通过疫苗接种仍然是预防疾病的可靠手段。对于活疫苗病毒,存在一个问题,即病毒疫苗的溢出可能导致将转基因病毒引入自然界中可持续的虱-脊椎动物宿主传播周期。为了限制tick传播的黄病毒(Langat病毒,LGTV)载体的向性,我们将tick特异性microRNA(mir-1,mir-275和mir-279)的靶标序列单独或组合插入了LGTV基因组的多个遥远区域。这导致壁虱来源的细胞中病毒复制的选择性减弱。已开发出LGTV表达壁虱和脊椎动物CNS特异性miRNA靶序列的组合。产生的病毒有效复制,并在不表达这些miRNA的猿猴Vero细胞中保持稳定,但是受到严格限制,不能在壁虱来源的细胞中复制。此外,同时进行双重miRNA靶向治疗可导致活食蚁x中的病毒复制沉默,并消除高度允许的新生小鼠中的病毒神经向性。因此,在脊椎动物和无脊椎动物宿主中同时限制不良复制事件将确保活tick传病毒疫苗候选物的环境安全。

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