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酵母切割与聚腺苷酸化因子亚基Ydh1p/Cft2p在mRNA前体3'末端形成中的作用。

The role of the yeast cleavage and polyadenylation factor subunit Ydh1p/Cft2p in pre-mRNA 3'-end formation.

作者信息

Kyburz Andrea, Sadowski Martin, Dichtl Bernhard, Keller Walter

机构信息

Department of Cell Biology, Biozentrum, University of Basel, Klingelbergstrasse 70, CH-4056 Basel, Switzerland.

出版信息

Nucleic Acids Res. 2003 Jul 15;31(14):3936-45. doi: 10.1093/nar/gkg478.

Abstract

Cleavage and polyadenylation factor (CPF) is a multi-protein complex that functions in pre-mRNA 3'-end formation and in the RNA polymerase II (RNAP II) transcription cycle. Ydh1p/Cft2p is an essential component of CPF but its precise role in 3'-end processing remained unclear. We found that mutations in YDH1 inhibited both the cleavage and the polyadenylation steps of the 3'-end formation reaction in vitro. Recently, we demonstrated that an important function of CPF lies in the recognition of poly(A) site sequences and RNA binding analyses suggesting that Ydh1p/Cft2p interacts with the poly(A) site region. Here we show that mutant ydh1 strains are deficient in the recognition of the ACT1 cleavage site in vivo. The C-terminal domain (CTD) of RNAP II plays a major role in coupling 3'-end processing and transcription. We provide evidence that Ydh1p/Cft2p interacts with the CTD of RNAP II, several other subunits of CPF and with Pcf11p, a component of CF IA. We propose that Ydh1p/Cft2p contributes to the formation of important interaction surfaces that mediate the dynamic association of CPF with RNAP II, the recognition of poly(A) site sequences and the assembly of the polyadenylation machinery on the RNA substrate.

摘要

切割与聚腺苷酸化因子(CPF)是一种多蛋白复合物,在mRNA前体3'末端形成以及RNA聚合酶II(RNAP II)转录循环中发挥作用。Ydh1p/Cft2p是CPF的一个必需组分,但其在3'末端加工中的精确作用仍不清楚。我们发现YDH1中的突变在体外抑制了3'末端形成反应的切割和聚腺苷酸化步骤。最近,我们证明CPF的一个重要功能在于识别聚腺苷酸化位点序列,并且RNA结合分析表明Ydh1p/Cft2p与聚腺苷酸化位点区域相互作用。在此我们表明,在体内突变的ydh1菌株在识别ACT1切割位点方面存在缺陷。RNAP II的C末端结构域(CTD)在耦合3'末端加工与转录过程中起主要作用。我们提供证据表明Ydh1p/Cft2p与RNAP II的CTD、CPF的其他几个亚基以及CF IA的一个组分Pcf11p相互作用。我们提出Ydh1p/Cft2p有助于形成重要的相互作用表面,这些表面介导CPF与RNAP II的动态结合、聚腺苷酸化位点序列的识别以及聚腺苷酸化机制在RNA底物上的组装。

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