Literature DB >> 14645221

Histone acetyltransferase-dependent chromatin remodeling and the vascular clock.

Anne M Curtis1, Sang-beom Seo, Elizabeth J Westgate, Radu Daniel Rudic, Emer M Smyth, Debabrata Chakravarti, Garret A FitzGerald, Peter McNamara.   

Abstract

Rhythmic gene expression is central to the circadian control of physiology in mammals. Transcriptional activation of Per and Cry genes by heterodimeric bHLH-PAS proteins is a key event in the feedback loop that drives rhythmicity; however, the mechanism is not clearly understood. Here we show the transcriptional coactivators and histone acetyltransferases, p300/CBP, PCAF, and ACTR associate with the bHLH-PAS proteins, CLOCK and NPAS2, to regulate positively clock gene expression. Furthermore, Cry2 mediated repression of NPAS2:BMAL1 is overcome by overexpression of p300 in transactivation assays. Accordingly, p300 exhibits a circadian time-dependent association with NPAS2 in the vasculature, which precedes peak expression of target genes. In addition, a rhythm in core histone H3 acetylation on the mPer1 promoter in vivo correlates with the cyclical expression of their mRNAs. Temporal coactivator recruitment and HAT-dependent chromatin remodeling on the promoter of clock controlled genes in the vasculature permits the mammalian clock to orchestrate circadian gene expression.

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Year:  2003        PMID: 14645221     DOI: 10.1074/jbc.M311973200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  82 in total

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Journal:  Cell Rep       Date:  2014-02-13       Impact factor: 9.423

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10.  High-throughput screening and chemical biology: new approaches for understanding circadian clock mechanisms.

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