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Human La binds mRNAs through contacts to the poly(A) tail

机译:人类La通过与poly(A)尾巴接触而结合mRNA

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摘要

In addition to a role in the processing of nascent RNA polymerase III transcripts, La proteins are also associated with promoting cap-independent translation from the internal ribosome entry sites of numerous cellular and viral coding RNAs. La binding to RNA polymerase III transcripts via their common UUU-3’OH motif is well characterized, but the mechanism of La binding to coding RNAs is poorly understood. Using electromobility shift assays and cross-linking immunoprecipitation, we show that in addition to a sequence specific UUU-3’OH binding mode, human La exhibits a sequence specific and length dependent poly(A) binding mode. We demonstrate that this poly(A) binding mode uses the canonical nucleic acid interaction winged helix face of the eponymous La motif, previously shown to be vacant during uridylate binding. We also show that cytoplasmic, but not nuclear La, engages poly(A) RNA in human cells, that La entry into polysomes utilizes the poly(A) binding mode, and that La promotion of translation from the cyclin D1 internal ribosome entry site occurs in competition with cytoplasmic poly(A) binding protein (PABP). Our data are consistent with human La functioning in translation through contacts to the poly(A) tail.
机译:La蛋白除了在新生RNA聚合酶III转录物的加工中发挥作用外,还与促进来自许多细胞和病毒编码RNA的内部核糖体进入位点的不依赖帽的翻译有关。 La通过其共同的UUU-3’OH基序与RNA聚合酶III转录物结合的特征已得到很好的表征,但对La与编码RNA结合的机理了解甚少。使用电动迁移率分析和交联免疫沉淀,我们显示,除了序列特异性的UUU-3’OH结合模式之外,人La还具有序列特异性和长度依赖性的poly(A)结合模式。我们证明此poly(A)绑定模式使用同名的La主题的规范的核酸相互作用翼翅的螺旋面,以前显示在尿嘧啶结合期间是空的。我们还显示,细胞质而不是核La参与人类细胞中的poly(A)RNA,La进入多核糖体利用poly(A)结合模式,并且发生La促进细胞周期蛋白D1内部核糖体进入位点的翻译与细胞质聚(A)结合蛋白(PABP)竞争。我们的数据与人类La通过与poly(A)尾巴的接触而在翻译中发挥作用相一致。

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