首页> 外文期刊>The Journal of General Virology: A Federation of European Miorobiological Societies Journal >Avian metapneumovirus SH gene end and G protein mutations influence the level of protection of live-vaccine candidates
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Avian metapneumovirus SH gene end and G protein mutations influence the level of protection of live-vaccine candidates

机译:禽偏肺病毒SH基因末端和G蛋白突变影响候选活疫苗的保护水平

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A prototype avian metapneumovirus (AMPV) vaccine (P20) was previously shown to give variable outcomes in experimental trials. Following plaque purification, three of 12 viruses obtained from P20 failed to induce protection against virulent challenge, whilst the remainder retained their protective capacity. The genome sequences of two protective viruses were identical to the P20 consensus, whereas two non-protective viruses differed only in the SH gene transcription termination signal. Northern blotting showed that the alterations in the SH gene-end region of the non-protective viruses led to enhanced levels of dicistronic mRNA produced by transcriptional readthrough. A synthetic minigenome was used to demonstrate that the altered SH gene-end region reduced the level of protein expression from a downstream gene. The genomes of the remaining eight plaque-purified viruses were sequenced in the region where the P20 consensus sequence differed from the virulent progenitor. The seven protective clones were identical, whereas the non-protective virus retained the virulent progenitor sequence at two positions and contained extensive alterations in its attachment (G) protein sequence associated with a reduced or altered expression pattern of G protein on Western blots. The data indicate that the efficacy of a putative protective vaccine strain is affected by mutations altering the balance of G protein expression.
机译:原型禽偏肺病毒 (AMPV) 疫苗 (P20) 先前在实验试验中被证明会产生不同的结果。斑块纯化后,从 P20 获得的 12 种病毒中有 3 种未能诱导对毒力攻击的保护,而其余病毒保留了它们的保护能力。两种保护性病毒的基因组序列与P20共识相同,而两种非保护性病毒仅在SH基因转录终止信号上有所不同。Northern印迹显示,非保护性病毒SH基因末端区域的改变导致转录通读产生的二分子mRNA水平升高。合成的微基因组用于证明改变的 SH 基因末端区域降低了下游基因的蛋白质表达水平。其余8种斑块纯化病毒的基因组在P20共识序列与致病祖细胞不同的区域进行测序。七个保护性克隆是相同的,而非保护性病毒在两个位置保留了毒力祖细胞序列,并且其附着(G)蛋白序列存在广泛的改变,这与蛋白质印迹上G蛋白的表达模式减少或改变有关。数据表明,推定的保护性疫苗株的功效受到改变G蛋白表达平衡的突变的影响。

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