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RNA 聚合酶 III 复合物的组装涉及一个假定的共翻译机制。

Assembly of RNA polymerase III complex involves a putative co-translational mechanism.

机构信息

Laboratory of tRNA Transcription, Institute of Biochemistry and Biophysics, Polish Academy of Sciences, Pawińskiego 5A, 02-106 Warsaw, Poland.

出版信息

Gene. 2022 May 25;824:146394. doi: 10.1016/j.gene.2022.146394. Epub 2022 Mar 9.

Abstract

Detailed knowledge of structures of yeast RNA polymerases (RNAPs) contrasts with the limited information that is available on the control of their assembly. RNAP enzymes are large heteromeric complexes that function in the nucleus, but they are assembled in the cytoplasm and imported to the nucleus with help from specific auxiliary factors. Here, I review a recent study that suggests that the formation of an early-stage assembly intermediate of the RNAP III complex occurs through a co-translational mechanism. According to our hypothesis, RNAP III assembly might be seeded while the Rpb10 subunit of the enzyme core is being synthesized by cytoplasmic ribosome machinery. The co-translational assembly of RNAP III is mediated by Rbs1 protein which binds to 3'-untranslated regions in mRNA in a way that depends on the R3H domain in the Rbs1 sequence.

摘要

详细了解酵母 RNA 聚合酶(RNAP)的结构与对其组装控制的有限信息形成鲜明对比。RNAP 酶是在核内发挥功能的大型异源聚合酶复合物,但它们在细胞质中组装,并在特定辅助因子的帮助下被运送到核内。在这里,我回顾了一项最近的研究,该研究表明,RNAP III 复合物的早期组装中间产物的形成是通过共翻译机制发生的。根据我们的假设,在细胞质核糖体机制合成酶核心的 Rpb10 亚基时,RNAP III 的组装可能就已经开始了。Rbs1 蛋白介导 RNAP III 的共翻译组装,该蛋白以依赖于 Rbs1 序列中的 R3H 结构域的方式与 mRNA 的 3'-非翻译区结合。

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