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Ty1 整合酶与 RNA 聚合酶 III 结合的结构基础,用于靶向逆转录转座子的整合。

Structural basis of Ty1 integrase tethering to RNA polymerase III for targeted retrotransposon integration.

机构信息

Centro de Investigaciones Biológicas Margarita Salas, CSIC, 28040, Madrid, Spain.

Aix-Marseille Université, CNRS, AFMB UMR 7257, 13288, Marseille, France.

出版信息

Nat Commun. 2023 Mar 28;14(1):1729. doi: 10.1038/s41467-023-37109-4.

Abstract

The yeast Ty1 retrotransposon integrates upstream of genes transcribed by RNA polymerase III (Pol III). Specificity of integration is mediated by an interaction between the Ty1 integrase (IN1) and Pol III, currently uncharacterized at the atomic level. We report cryo-EM structures of Pol III in complex with IN1, revealing a 16-residue segment at the IN1 C-terminus that contacts Pol III subunits AC40 and AC19, an interaction that we validate by in vivo mutational analysis. Binding to IN1 associates with allosteric changes in Pol III that may affect its transcriptional activity. The C-terminal domain of subunit C11, involved in RNA cleavage, inserts into the Pol III funnel pore, providing evidence for a two-metal mechanism during RNA cleavage. Additionally, ordering next to C11 of an N-terminal portion from subunit C53 may explain the connection between these subunits during termination and reinitiation. Deletion of the C53 N-terminal region leads to reduced chromatin association of Pol III and IN1, and a major fall in Ty1 integration events. Our data support a model in which IN1 binding induces a Pol III configuration that may favor its retention on chromatin, thereby improving the likelihood of Ty1 integration.

摘要

酵母 Ty1 反转录转座子整合到 RNA 聚合酶 III(Pol III)转录的基因上游。整合的特异性由 Ty1 整合酶(IN1)和 Pol III 之间的相互作用介导,目前在原子水平上尚未阐明。我们报告了 Pol III 与 IN1 复合物的冷冻电镜结构,揭示了 IN1 C 端的 16 个残基片段与 Pol III 亚基 AC40 和 AC19 相互作用,通过体内突变分析验证了这种相互作用。与 IN1 的结合与 Pol III 的变构相关联,这可能影响其转录活性。参与 RNA 切割的亚基 C11 的 C 末端结构域插入 Pol III 漏斗孔中,为 RNA 切割过程中的双金属机制提供了证据。此外,亚基 C53 的 N 末端部分紧邻 C11 的排列可能解释了终止和重新起始过程中这些亚基之间的连接。C53 N 末端区域的缺失导致 Pol III 和 IN1 与染色质的关联减少,Ty1 整合事件大量减少。我们的数据支持这样一种模型,即 IN1 结合诱导 Pol III 构象,这可能有利于其在染色质上的保留,从而提高 Ty1 整合的可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/22fe/10050235/d90a444ec7e2/41467_2023_37109_Fig1_HTML.jpg

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