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Intra-host variation structure of classical swine fever virus NS5B in relation to antiviral therapy

机译:经典猪瘟病毒NS5B的宿主内变异结构与抗病毒治疗的关系

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Classical swine fever (CSF) is one of most important diseases of the Suidea with severe social economic consequences in case of outbreaks. Antivirals have been demonstrated, in recent publications, to be an interesting alternative method of fighting the disease. However, classical swine fever virus is an RNA virus which presents a challenge as intra-host variation and the error prone RNA dependent RNA poly-merase (RdRp) could lead to the emergence/selection of resistant variants hampering further treatment. Therefore, it was the purpose of this study to investigate the intra-host variation of the RdRp gene, targeted by antivirals, in respect to antiviral treatment. Using the non-unique nucleotide changes, a limited intra-host variation was found in the wild type virus with 2 silent and 2 non-synonymous sites. This number shifted significantly when an antiviral resistant variant was analyzed. In total 22 nt changes were found resulting in 14 amino acid changes whereby each genome copy contained at least 2 amino-acid changes in the RdRp. Interestingly, the frequency of the mutations situated in close proximity to a region involved in antiviral resistance in CSFV and bovine viral diarrhea virus (BVDV) was elevated compared to the other mutations. None of the identified mutations in the resistant variant and which could potentially result in antiviral resistance was present in the wild type virus as a non-unique mutation. In view of the spectrum of mutations identified in the resistance associated region and that none of the resistance associated mutations reported for another strain of classical swine fever for the same antiviral were observed in the study, it can be suggested that multiple mutations confer resistance to some degree. Although the followed classical approach allowed the analysis the RdRp as a whole, the contribution of unique mutations to the intra-host variation could not be completely resolved. There was a significant difference in de number of unique mutations found between: I/wild type virus and the antiviral resistant variant and 2/between both and the number to be expected from the error rate of the RT-PCR process. This indicates that the some of the unique mutations contributed to the intra-host variation and that the antiviral pressure also shifted this pattern. This is important as one of the non-synonymous mutations found in the resistant variant and which was located in the antiviral resistance associated region, was present in the wild type virus as a unique mutation. The findings presented in this study not only show the importance of intra-host variation analysis but also warrants further research certainly in view of the potential inclusion of antivirals in a control/eradication strategy.
机译:古典猪瘟(CSF)是Suidea最重要的疾病之一,一旦暴发,将给社会经济造成严重后果。在最近的出版物中,已经证明抗病毒药是对抗该疾病的一种有趣的替代方法。但是,经典的猪瘟病毒是一种RNA病毒,由于宿主内部变异而引起挑战,并且容易出错的依赖RNA的RNA聚合酶(RdRp)可能导致耐药变体的出现/选择,从而阻碍了进一步的治疗。因此,本研究的目的是针对抗病毒治疗,研究抗病毒药物靶向的RdRp基因的宿主内部变异。使用非唯一核苷酸变化,在野生型病毒中发现了有限的宿主内变异,具有2个沉默位点和2个非同义位点。当分析抗病毒抗性变体时,该数字发生了显着变化。总共发现22个核苷酸变化,导致14个氨基酸变化,从而每个基因组拷贝在RdRp中至少包含2个氨基酸变化。有趣的是,与其他突变相比,位于CSFV和牛病毒性腹泻病毒(BVDV)中与抗病毒抗性相关的区域非常接近的突变频率较高。在野生型病毒中,抗药性变异体中未鉴定出的可能会导致抗病毒抗药性的突变均以非唯一突变的形式存在。鉴于在抗药性相关区域鉴定出的突变谱,并且在研究中未观察到针对同一抗病毒的另一株经典猪瘟菌株报告的抗药性相关突变,因此可以认为多个突变赋予了某些抗药性度。尽管遵循的经典方法可以对RdRp进行整体分析,但不能完全解决独特突变对宿主内部变异的影响。在I /野生型病毒和抗病毒抗性变异之间以及在两者之间的独特突变数目之间存在显着差异,并且从RT-PCR过程的错误率可以预期的数目之间存在显着差异。这表明某些独特的突变导致宿主内部变异,而抗病毒压力也改变了这种模式。这很重要,因为在抗性变异体中发现并位于抗病毒抗性相关区域的非同义突变之一在野生型病毒中作为独特突变存在。这项研究中提出的发现不仅表明了宿主内部变异分析的重要性,而且鉴于在控制/根除策略中可能包含抗病毒药,因此肯定值得进一步研究。

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