首页> 外文期刊>Virology >A single nucleotide substitution in the transcription start signal of the M2 gene of respiratory syncytial virus vaccine candidate cpts248/404 is the major determinant of the temperature-sensitive and attenuation phenotypes.
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A single nucleotide substitution in the transcription start signal of the M2 gene of respiratory syncytial virus vaccine candidate cpts248/404 is the major determinant of the temperature-sensitive and attenuation phenotypes.

机译:呼吸道合胞病毒疫苗候选cpts248 / 404的M2基因的转录起始信号中的单核苷酸取代是温度敏感型和减毒表型的主要决定因素。

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Respiratory syncytial virus (RSV) cpts248/404 is a live-attenuated, temperature-sensitive (ts) vaccine candidate derived from cole-passaged cpRSV by two rounds of chemical mutagenesis and biological selection. Previous sequence analysis showed that these two steps introduced three single nucleotide substitutions into the cpRSV parent. Two of these occurred with the coding sequence for the L protein, and each resulted in a single amino acid substitution: Gin-831-Leu (248 mutation) and Asp-1183-Glu (404-L mutation). The third mutation resulted in a nucleotide substitution at position 9 of the c/s-acting gene start signal of the M2 gene (404-M2 mutation). In the present study, the genetic basis of attenuation of cpts248/404 was defined by the introduction of each of these mutations (singly or in combination) into a full-length cDNA clone of cpRSV. Recombinant RSV derived from each mutant cDNA was analyzed to determine the contribution of each mutation to the ts and attenuation phenotypes of the virus. This analysis showed that the 248 mutation specifies a significant reduction of plaque formation at 38 degrees and is responsible for an intermediate level of attenuation in mice. In contrast, the 404-L mutation did not contribute to the ts or attenuation phenotype alone or in combination with other mutations and is thus an incidental change. unexpectedly, the 404-M2 mutation alone specified complete restriction of plaque formation at 37 degrees C an a high level of attenuation in mice. This indicates that the level of temperature sensitivity and attenuation of cpts248/404 can be attributed primarily to the 404-M2 mutation. Thus the cpts248/404 virus contains a set of ts and non-ts attenuating mutations, which likely accounts for its genetic stability. The recombinant version of this virus, rA2cp248/404, was phenotypically indistinguishable from cpts248/404 and represents a background into which additional mutations can be introduced as needed to obtain the desired level of attenuation for successful immunization of the very young human infant.
机译:呼吸道合胞病毒(RSV)cpts248 / 404是通过两轮化学诱变和生物学筛选从经油菜的cpRSV衍生的减毒活体,温度敏感(ts)疫苗。先前的序列分析表明,这两个步骤将三个单核苷酸取代引入了cpRSV亲本。其中两个发生在L蛋白的编码序列上,每个导致一个氨基酸取代:Gin-831-Leu(248突变)和Asp-1183-Glu(404-L突变)。第三次突变导致M2基因c / s作用基因起始信号第9位的核苷酸取代(404-M2突变)。在本研究中,通过将每种突变(单独或组合)引入cpRSV的全长cDNA克隆中来定义cpts248 / 404减毒的遗传基础。分析源自每个突变体cDNA的重组RSV,以确定每个突变体对病毒的ts和减毒表型的贡献。这项分析表明248突变表明38度噬菌斑形成明显减少,并且是小鼠中度减毒的中间原因。相反,404-L突变单独或与其他突变结合时不会对ts或减毒表型产生影响,因此是偶然的变化。出乎意料的是,单独的404-M2突变规定了在37摄氏度时斑块形成的完全限制,这在小鼠中是高度减毒的。这表明cpts248 / 404的温度敏感性和衰减水平主要归因于404-M2突变。因此,cpts248 / 404病毒包含一组ts和非ts减毒突变,这可能是其遗传稳定性的原因。该病毒的重组版本rA2cp248 / 404在表型上与cpts248 / 404不能区分,并且代表了可以根据需要引入其他突变以获得所需的减毒水平以成功免疫非常年轻的婴儿的背景。

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