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The S2 gene nucleotide sequences of prototype strains of the three reovirus serotypes: characterization of reovirus core protein sigma 2.

机译:三种呼肠孤病毒血清型原型菌株的S2基因核苷酸序列:呼肠孤病毒核心蛋白sigma 2的表征。

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摘要

The S2 gene nucleotide sequences of prototype strains of the three reovirus serotypes were determined to gain insight into the structure and function of the S2 translation product, virion core protein sigma 2. The S2 sequences of the type 1 Lang, type 2 Jones, and type 3 Dearing strains are 1,331 nucleotides in length and contain a single large open reading frame that could encode a protein of 418 amino acids, corresponding to sigma 2. The deduced sigma 2 amino acid sequences of these strains are very conserved, being identical at 94% of the sequence positions. Predictions of sigma 2 secondary structure and hydrophobicity suggest that the protein has a two-domain structure. A larger domain is suggested to be formed from the amino-terminal three-fourths of sigma 2 sequence, which is separated from a smaller carboxy-terminal domain by a turn-rich hinge region. The carboxy-terminal domain includes sequences that are more hydrophilic than those in the rest of the protein and contains sequences which are predicted to form an alpha-helix. A region of striking similarity was found between amino acids 354 and 374 of sigma 2 and amino acids 1008 and 1031 of the beta subunit of the Escherichia coli DNA-dependent RNA polymerase. We suggest that the regions with similar sequence in sigma 2 and the beta subunit form amphipathic alpha-helices which may play a related role in the function of each protein. We have also performed experiments to further characterize the double-stranded RNA-binding activity of sigma 2 and found that the capacity to bind double-stranded RNA is a property of the sigma 2 protein of prototype strains and of the S2 mutant tsC447.
机译:确定了三种呼肠孤病毒血清型原型菌株的S2基因核苷酸序列,以深入了解S2翻译产物病毒体核心蛋白sigma 2的结构和功能。1型Lang,2型Jones和2型S2序列。 3亲爱的菌株长度为1,331个核苷酸,并包含一个大的可读框,可编码418个氨基酸的蛋白质,对应于sigma2。推导的这些菌株的sigma 2氨基酸序列非常保守,相同程度为94%序列位置。 σ2二级结构和疏水性的预测表明该蛋白质具有两个域结构。建议从sigma 2序列的氨基末端四分之三形成一个较大的结构域,该序列与一个较小的羧基末端结构域通过一个富含转角的铰链区隔开。羧基末端结构域包含比蛋白质其余部分亲水的序列,并包含预计形成α-螺旋的序列。在大肠杆菌DNA依赖性RNA聚合酶的sigma 2氨基酸354和374与β亚基的氨基酸1008和1031之间发现了惊人相似的区域。我们建议在sigma 2和beta亚基中具有相似序列的区域形成两亲性α螺旋,其可能在每种蛋白质的功能中发挥相关作用。我们还进行了实验,以进一步表征sigma 2的双链RNA结合活性,并发现结合双链RNA的能力是原型菌株和S2突变tsC447的sigma 2蛋白的特性。

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