Proteomics

Dataset Information

0

: Arginine methylation of BRD4 by PRMT2/4 governs transcription and DNA repair


ABSTRACT: BRD4 functions as an epigenetic reader and plays a crucial role in regulating transcription and genome stability. Dysregulation of BRD4 is frequently observed in various human cancers. However, the molecular details of BRD4 regulation remain largely unknown. Here, we report that PRMT2- and PRMT4-mediated arginine methylation is pivotal for BRD4-dependent transcription, DNA repair, and tumor growth. Specifically, PRMT2/4 interact with and methylates BRD4 at R179, R181, and R183. This arginine methylation selectively controls a transcriptional program by promoting BRD4 enrichment at the hyper-acetylated chromatin regions. Moreover, BRD4 arginine methylation is induced by DNA damage and thereby promotes its binding to chromatin for DNA repair. Deficiency in BRD4 arginine methylation significantly suppresses tumor growth and sensitizes cells to BET inhibitors and DNA damaging agents. Therefore, our findings reveal an arginine methylation-dependent regulatory mechanism of BRD4 function and highlight targeting PRMT2/4 for better anti-tumor effect of BET inhibitors and DNA damaging agents.

INSTRUMENT(S): Orbitrap Fusion Lumos

ORGANISM(S): Homo Sapiens (human)

SUBMITTER: Jennifer Bethard  

LAB HEAD: Wenjian Gan, Ph.D.

PROVIDER: PXD034650 | Pride | 2023-03-11

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
01112022_Gan_noGluC-04.msf Msf
01112022_Gan_noGluC.raw Raw
01272022_Gan_BRD4_GluC.raw Raw
BRD4.fasta Fasta
Methyl__KR_Sites.txt Txt
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Publications

Arginine methylation of BRD4 by PRMT2/4 governs transcription and DNA repair.

Liu Liu L   Lin Baicheng B   Yin Shasha S   Ball Lauren E LE   Delaney Joe R JR   Long David T DT   Gan Wenjian W  

Science advances 20221207 49


BRD4 functions as an epigenetic reader and plays a crucial role in regulating transcription and genome stability. Dysregulation of BRD4 is frequently observed in various human cancers. However, the molecular details of BRD4 regulation remain largely unknown. Here, we report that PRMT2- and PRMT4-mediated arginine methylation is pivotal for BRD4 functions on transcription, DNA repair, and tumor growth. Specifically, PRMT2/4 interacts with and methylates BRD4 at R179, R181, and R183. This arginine  ...[more]

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