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Modulation of gene expression dynamics by co-transcriptional histone methylations
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Title
Modulation of gene expression dynamics by co-transcriptional histone methylations
Issued Date
2017-04
Citation
Experimental & Molecular Medicine, v.49, no.4
Type
Article
Keywords
RNA-POLYMERASE-IISACCHAROMYCES-CEREVISIAEH3K4 METHYLATIONCODING REGIONSACETYLTRANSFERASE COMPLEXANTISENSE TRANSCRIPTIONDEACETYLASE COMPLEXH2B UBIQUITYLATIONSET2 METHYLATIONK-36 METHYLATION
ISSN
1226-3613
Abstract
Co-transcriptional methylations of histone H3 at lysines 4 and 36, highly conserved methyl marks from yeast to humans, have profound roles in regulation of histone acetylation. These modifications function to recruit and/or activate distinct histone acetyltransferases (HATs) or histone deacetylases (HDACs). Whereas H3K4me3 increases acetylation at promoters via multiple HATs, H3K4me2 targets Set3 HDAC to deacetylate histones in 5' transcribed regions. In 3' regions of genes, H3K36me2/3 facilitates deacetylation by Rpd3S HDAC and slows elongation. Despite their important functions in deacetylation, no strong effects on global gene expression have been seen under optimized or laboratory growth conditions. Instead, H3K4me2-Set3 HDAC and Set2-Rpd3S pathways primarily delay the kinetics of messenger RNA (mRNA) and long noncoding RNA (lncRNA) induction upon environmental changes. A majority of mRNA genes regulated by these pathways have an overlapping lncRNA transcription either from an upstream or an antisense promoter. Surprisingly, the distance between mRNA and lncRNA promoters seems to specify the repressive effects of the two pathways. Given that co-transcriptional methylations and acetylation have been linked to many cancers, studying their functions in a dynamic condition or during cancer progression will be much more important and help identify novel genes associated with cancers.
URI
http://hdl.handle.net/20.500.11750/4202
DOI
10.1038/emm.2017.19
Publisher
생화학분자생물학회
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이성배
Lee, Sung Bae이성배

Department of Brain Sciences

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