Published July 17, 2017
| Version v1
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A sequence level model of an intact locus predicts the location and function of nonadditive enhancers
Description
Metazoan gene expression is controlled through the action of long stretches of noncoding DNA that contain enhancers—shorter sequences responsible for controlling a single aspect of a gene's expression pattern. Models built on thermodynamics have shown how enhancers interpret protein concentration in order to determine specific levels of gene expression, but the emergent regulatory logic of a complete regulatory locus shows qualitative and quantitative differences from isolated enhancers. Such differences may arise from steric competition limiting the quantity of DNA that can simultaneously influence the transcription machinery. We incorporated this competition into a mechanistic model of gene regulation, generated efficient algorithms for this computation, and applied it to the regulation of Drosophila even-skipped (eve). This model finds the location of enhancers and identifies which factors control the boundaries of eve expression. This model predicts a new enhancer that, when assayed in vivo, drives expression in a non-eve pattern. Incorporation of chromatin accessibility eliminates this inconsistency.
Data availability
Transcription factor fluorescence measurements used in this paper are publicly available from the authors at http://flyex.uchicago.edu/flyex/ and are also available at figshare https://doi.org/10.6084/m9.figshare.5146231.v1). Third-party PWMs used in this work are publicly available at http://mccb.umassmed.edu/ffs/ and http://line.bioinfolab.net/webgate/help/dxp.htm#D-stat-223. The code generated for this work is available at github.com/kennethabarr. All other relevant data are within the paper and its Supporting Information files.
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Additional details
Identifiers
- DOI
- 10.1371/journal.pone.0180861
- Other
- oai:uchicago.tind.io:6635
Funding
- National Institutes of Health
- R01 OD010936
- University of Chicago