Transcription Directionality is Licensed by Integrator at Active Human Promoters

Overview

Journal Nat Struct Mol Biol

Specialties Cell Biology
Molecular Biology

Date 2024 Apr 22

PMID 38649617

Authors

Jiao Yang

Jingyang Li

Langxi Miao

Xu Gao

Wenhao Sun

Shuo Linghu

Guiping Ren

Bangya Peng

Shunkai Chen

Zhongqi Liu

Bo Wang

Ao Dong

Duo Huang

Jinrong Yuan

Yunkun Dang

Fan Lai

Affiliations

Soon will be listed here.

Abstract

A universal characteristic of eukaryotic transcription is that the promoter recruits RNA polymerase II (RNAPII) to produce both precursor mRNAs (pre-mRNAs) and short unstable promoter upstream transcripts (PROMPTs) toward the opposite direction. However, how the transcription machinery selects the correct direction to produce pre-mRNAs is largely unknown. Here, through multiple acute auxin-inducible degradation systems, we show that rapid depletion of an RNAPII-binding protein complex, Integrator, results in robust PROMPT accumulation throughout the genome. Interestingly, the accumulation of PROMPTs is compensated by the reduction of pre-mRNA transcripts in actively transcribed genes. Consistently, Integrator depletion alters the distribution of polymerase between the sense and antisense directions, which is marked by increased RNAPII-carboxy-terminal domain Tyr1 phosphorylation at PROMPT regions and a reduced Ser2 phosphorylation level at transcription start sites. Mechanistically, the endonuclease activity of Integrator is critical to suppress PROMPT production. Furthermore, our data indicate that the presence of U1 binding sites on nascent transcripts could counteract the cleavage activity of Integrator. In this process, the absence of robust U1 signal at most PROMPTs allows Integrator to suppress the antisense transcription and shift the transcriptional balance in favor of the sense direction.

Citing Articles

Human promoter directionality is determined by transcriptional initiation and the opposing activities of INTS11 and CDK9.

Eaton J, Board J, Davidson L, Estell C, West S Elife. 2024; 13.

PMID: 38976490 PMC: 11230626. DOI: 10.7554/eLife.92764.

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