Enhancer transcription: what, where, when, and why?
- PMID: 29440223
- PMCID: PMC5828389
- DOI: 10.1101/gad.311605.118
Enhancer transcription: what, where, when, and why?
Abstract
Following the discovery of widespread enhancer transcription, enhancers and promoters have been found to be far more similar than previously thought. In this issue of Genes & Development, two studies (Henriques and colleagues [pp. 26-41] and Mikhaylichenko and colleagues [pp. 42-57]) shine new light on the transcriptional nature of promoters and enhancers in Drosophila Together, these studies support recent work in mammalian cells that indicates that most active enhancers drive local transcription using factors and mechanisms similar to those of promoters. Intriguingly, enhancer transcription is shown to be coordinated by SPT5- and P-TEFb-mediated pause-release, but the pause half-life is shorter, and termination is more rapid at enhancers than at promoters. Moreover, bidirectional transcription from promoters is associated with enhancer activity, lending further credence to models in which regulatory elements exist along a spectrum of promoter-ness and enhancer-ness. We propose a general unified model to explain possible functions of transcription at enhancers.
Keywords: P-TEFb; eRNA; embryonic development; enhancers; promoters; superenhancers; termination; transcription.
© 2018 Tippens et al.; Published by Cold Spring Harbor Laboratory Press.
Comment on
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Widespread transcriptional pausing and elongation control at enhancers.Genes Dev. 2018 Jan 1;32(1):26-41. doi: 10.1101/gad.309351.117. Epub 2018 Jan 29. Genes Dev. 2018. PMID: 29378787 Free PMC article.
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The degree of enhancer or promoter activity is reflected by the levels and directionality of eRNA transcription.Genes Dev. 2018 Jan 1;32(1):42-57. doi: 10.1101/gad.308619.117. Epub 2018 Jan 29. Genes Dev. 2018. PMID: 29378788 Free PMC article.
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