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A Role for the Sendai Virus P Protein Trimer in RNA Synthesis

机译:仙台病毒P蛋白三聚体在RNA合成中的作用

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摘要

The SeV P protein is found as a homotrimer (P3) when it is expressed in mammalian cells, and trimerization is mediated by a predicted coiled-coil motif which maps within amino acids (aa) 344 to 411 (the BoxA region). The bacterially expressed protein also appears to be trimeric, apparently precluding a role for phosphorylation in the association of the P monomers. I have examined the role of P trimerization both in the protein’s interaction with the nucleocapsid (N:RNA) template and in the protein’s function on the template during RNA synthesis. As with the results of earlier experiments (32), I found that both the BoxA and BoxC (aa 479 to 568) regions were required for stable binding of P to the N:RNA. Binding was also observed with P proteins containing less than three BoxC regions, suggesting that trimerization may be required to permit contacts between multiple BoxC regions and the N:RNA. However, these heterologous trimers failed to function in viral RNA synthesis, indicating that the third C-terminal leg of the trimer plays an essential role in P function on the template. We speculate that this function may involve the movement of P (and possibly the polymerase complex) on the template and the maintenance of processivity.
机译:当在哺乳动物细胞中表达时,发现SeV P蛋白是同型三聚体(P3),并且三聚化由预测的卷曲螺旋基序介导,该卷曲螺旋基序在氨基酸(aa)344至411(BoxA区)内定位。细菌表达的蛋白质也似乎是三聚体,显然排除了在P单体缔合中磷酸化的作用。我已经研究了P三聚化在蛋白质与核衣壳(N:RNA)模板的相互作用以及蛋白质在RNA合成过程中在模板上的功能中的作用。与早期实验的结果一样(32),我发现BoxA和BoxC(aa 479至568)区域都是P与N:RNA稳定结合所必需的。还观察到与包含少于三个BoxC区域的P蛋白的结合,表明可能需要三聚以允许多个BoxC区域与N:RNA之间接触。但是,这些异源三聚体不能在病毒RNA合成中起作用,表明该三聚体的第三C末端分支在模板上的P功能中起着至关重要的作用。我们推测此功能可能涉及模板上P(可能还有聚合酶复合物)的移动以及维持合成能力。

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