Histone Methylation-dependent Mechanisms Impose Ligand Dependency for Gene Activation by Nuclear Receptors

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2007 Feb 10

PMID 17289570

Citations 246

Authors

Ivan Garcia-Bassets

Young-Soo Kwon

Francesca Telese

Gratien G Prefontaine

Kasey R Hutt

Christine S Cheng

Bong-Gun Ju

Kenneth A Ohgi

Jianxun Wang

Laure Escoubet-Lozach

David W Rose

Christopher K Glass

Xiang-Dong Fu

Michael G Rosenfeld

Affiliations

Soon will be listed here.

Abstract

Nuclear receptors undergo ligand-dependent conformational changes that are required for corepressor-coactivator exchange, but whether there is an actual requirement for specific epigenetic landmarks to impose ligand dependency for gene activation remains unknown. Here we report an unexpected and general strategy that is based on the requirement for specific cohorts of inhibitory histone methyltransferases (HMTs) to impose gene-specific gatekeeper functions that prevent unliganded nuclear receptors and other classes of regulated transcription factors from binding to their target gene promoters and causing constitutive gene activation in the absence of stimulating signals. This strategy, based at least in part on an HMT-dependent inhibitory histone code, imposes a requirement for specific histone demethylases, including LSD1, to permit ligand- and signal-dependent activation of regulated gene expression. These events link an inhibitory methylation component of the histone code to a broadly used strategy that circumvents pathological constitutive gene induction by physiologically regulated transcription factors.

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