首页> 外文期刊>Nucleic Acids Research >RNA binding characteristics and overall topology of the vaccinia poly(A) polymerase-processivity factor-primer complex.
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RNA binding characteristics and overall topology of the vaccinia poly(A) polymerase-processivity factor-primer complex.

机译:牛痘聚(A)聚合酶-加工因子-引物复合物的RNA结合特征和整体拓扑。

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The vaccinia virus-encoded heterodimer responsible for poly(A) tail elongation comprises a polyadenylylation catalytic subunit (VP55) and associated processivity factor (VP39). We show that monomeric VP39's affinity for RNA homopolymers follows the hierarchy poly(I) >poly(U) poly(G) >poly(A) >poly(C), that the heterodimer interacts stably with 40-45 nucleotide nucleic acid segments, and that its homopolymer preference for polyadenylylation priming is comparable to the VP39 affinity hierarchy (above). For oligonucleotide ligands possessing the previously-identified (rU)2-(N)25-rU heterodimer-binding motif, the heterodimer's affinity and base-type preference are mediated via both the (rU)2and rU portions, with the greater contribution coming from (rU)2. VP39's R107 sidechain contributes to specificity at the downstream rU. Substitution of each ribouridylate of the motif with either ribothymidine or 4-thiodeoxythymidine indicated that the downstream rU interacts with both heterodimer subunits, whereas the upstream (rU)2interacts only with VP55. A 'crosslinking SELEX' approach indicated VP39-base proximity around position -10 of a 4-thioribouridine/deoxycytidine ligand pool. Upon incubating the heterodimer with a panel of identical-sequence oligonucleotides derivatized with azidophenacyl bromide at various phosphate positions, those derivatized at positions -11 to -21 photocrosslinked to both subunits in a coordinated manner. This region may therefore pass through a 'cleft' or enclosed 'channel' at the subunit interface.
机译:牛痘病毒编码的异聚二聚体,负责poly(A)尾巴的延伸,包含一个聚腺苷酸化催化亚基(VP55)和相关的持续合成因子(VP39)。我们显示单体VP39对RNA均聚物的亲和力遵循以下层次结构poly(I)> poly(U) poly(G)> poly(A)> poly(C),即异二聚体与40-45个核苷酸核酸稳定相互作用片段,并且其均聚物对聚腺苷酰化引发的偏好可与VP39亲和力等级相比(上图)。对于具有先前确定的(rU)2-(N)25-rU异二聚体结合基序的寡核苷酸配体,异二聚体的亲和力和碱基类型偏好是通过(rU)2和rU部分介导的,其中更大的贡献来自(rU)2。 VP39的R107侧链有助于下游rU的特异性。用核糖嘧啶核苷或4-硫代脱氧胸苷取代基序的每个核糖基磺酸盐表明,下游rU与两个异二聚体亚基相互作用,而上游(rU)2仅与VP55相互作用。 “交联SELEX”方法表明在4-硫代布丁烷/脱氧胞苷配体池的-10位附近有VP39碱基邻近。将异二聚体与一组在不同磷酸盐位置被叠氮苯甲酰溴衍生的相同序列的寡核苷酸孵育后,那些在位置-11至-21衍生的寡核苷酸以协调的方式光交联到两个亚基。因此,该区域可以在子单元界面处穿过“裂缝”或封闭的“通道”。

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