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Structure and Function of Pre-mRNA 5′-End CappingQuality Control and 3′-End Processing

机译:前mRNA 5-端帽的结构和功能质量控制和3端处理

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摘要

Messenger RNA precursors (pre-mRNAs) are produced as the nascent transcripts of RNA polymerase II (Pol II) in eukaryotes and must undergo extensive maturational processing, including 5′-end capping, splicing, and 3′-end cleavage and polyadenylation. This review will summarize the structural and functional information reported over the past few years on the large machinery required for the 3′-end processing of most pre-mRNAs, as well as the distinct machinery for the 3′-end processing of replication-dependent histone pre-mRNAs, which have provided great insights into the proteins and their subcomplexes in these machineries. Structural and biochemical studies have also led to the identification of a new class of enzymes (the DXO family enzymes) with activity toward intermediates of the 5′-end capping pathway. Functional studies demonstrate that these enzymes are part of a novel quality surveillance mechanism for pre-mRNA 5′-end capping. Incompletely capped pre-mRNAs are produced in yeast and human cells, in contrast to the general belief in the field that cappingalways proceeds to completion, and incomplete capping leads to defectsin splicing and 3′-end cleavage in human cells. The DXO familyenzymes are required for the detection and degradation of these defectiveRNAs.
机译:信使RNA前体(pre-mRNA)是真核生物中RNA聚合酶II(Pol II)的新生转录产物,必须经过广泛的成熟加工,包括5'-末端加帽,剪接和3'-末端裂解和聚腺苷酸化。这篇综述将总结过去几年报告的有关大多数pre-mRNA的3'末端加工所需的大型机器的结构和功能信息,以及与复制相关的3'末端加工的独特机器组蛋白前mRNA,为这些机器中的蛋白质及其亚复合物提供了深刻的见识。结构和生化研究也已导致鉴定出一类新的酶(DXO家族酶),该酶对5'端帽化途径的中间体具有活性。功能研究表明,这些酶是mRNA前5'端封端的新型质量监控机制的一部分。与在酵母和人类细胞中产生的不完全加帽的前mRNA相比,人们普遍认为加帽总是进行到完成,并且不完整的封盖会导致缺陷在人类细胞中的剪接和3'端切割。 DXO系列这些缺陷的检测和降解需要酶RNA。

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