SLAM-seq Defines Direct Gene-regulatory Functions of the BRD4-MYC Axis

Overview

Journal Science

Specialty Science

Date 2018 Apr 7

PMID 29622725

Citations 164

Authors

Matthias Muhar

Anja Ebert

Tobias Neumann

Christian Umkehrer

Julian Jude

Corinna Wieshofer

Philipp Rescheneder

Jesse J Lipp

Veronika A Herzog

Brian Reichholf

David A Cisneros

Thomas Hoffmann

Moritz F Schlapansky

Pooja Bhat

Arndt von Haeseler

Thomas Kocher

Anna C Obenauf

Johannes Popow

Stefan L Ameres

Johannes Zuber

Affiliations

Soon will be listed here.

Abstract

Defining direct targets of transcription factors and regulatory pathways is key to understanding their roles in physiology and disease. We combined SLAM-seq [thiol(SH)-linked alkylation for the metabolic sequencing of RNA], a method for direct quantification of newly synthesized messenger RNAs (mRNAs), with pharmacological and chemical-genetic perturbation in order to define regulatory functions of two transcriptional hubs in cancer, BRD4 and MYC, and to interrogate direct responses to BET bromodomain inhibitors (BETis). We found that BRD4 acts as general coactivator of RNA polymerase II-dependent transcription, which is broadly repressed upon high-dose BETi treatment. At doses triggering selective effects in leukemia, BETis deregulate a small set of hypersensitive targets including MYC. In contrast to BRD4, MYC primarily acts as a selective transcriptional activator controlling metabolic processes such as ribosome biogenesis and de novo purine synthesis. Our study establishes a simple and scalable strategy to identify direct transcriptional targets of any gene or pathway.

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