Anna Ebert scite author profile

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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Noch online? Studierendenbefragung zur medientechnischen Ausstattung - Gesamtbericht: Ergebnisse der universitätsweiten UDE-Umfrage im Sommersemester 2020

Stammen¹,

Ebert²

2021

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Lehre auf Distanz

Stammen¹,

Ebert²

2022

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Der Übergang vom Bachelor zum Master. Eine neue Schwelle der Bildungsbenachteiligung?

Ebert¹,

Stammen²

2014

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Studentischer Arbeitsaufwand für Studienprojekte

Dauner

Ebert

Grosche

et al. 2018

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Anna Ebert

SLAM-seq defines direct gene-regulatory functions of the BRD4-MYC axis

Noch online? Studierendenbefragung zur medientechnischen Ausstattung - Gesamtbericht: Ergebnisse der universitätsweiten UDE-Umfrage im Sommersemester 2020

Lehre auf Distanz

Der Übergang vom Bachelor zum Master. Eine neue Schwelle der Bildungsbenachteiligung?

Studentischer Arbeitsaufwand für Studienprojekte

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