Histone Deimination Antagonizes Arginine Methylation

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2004 Sep 2

PMID 15339660

Citations 296

Authors

Graeme L Cuthbert

Sylvain Daujat

Andrew W Snowden

Hediye Erdjument-Bromage

Teruki Hagiwara

Michiyuki Yamada

Robert Schneider

Philip D Gregory

Paul Tempst

Andrew J Bannister

Tony Kouzarides

Affiliations

Soon will be listed here.

Abstract

Methylation of arginine residues within histone H3 has been linked to active transcription. This modification appears on the estrogen-regulated pS2 promoter when the CARM1 methyltransferase is recruited during transcriptional activation. Here we describe a process, deimination, that converts histone arginine to citrulline and antagonizes arginine methylation. We show that peptidyl arginine deiminase 4 (PADI4) specifically deiminates, arginine residues R2, R8, R17, and R26 in the H3 tail. Deimination by PADI4 prevents arginine methylation by CARM1. Dimethylation of arginines prevents deimination by PADI4 although monomethylation still allows deimination to take place. In vivo targeting experiments on an endogenous promoter demonstrate that PADI4 can repress hormone receptor-mediated gene induction. Consistent with a repressive role for PADI4, this enzyme is recruited to the pS2 promoter following hormone induction when the gene is transcriptionally downregulated. The recruitment of PADI4 coincides with deimination of the histone H3 N-terminal tail. These results define deimination as a novel mechanism for antagonizing the transcriptional induction mediated by arginine methylation.

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