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Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle. | LitMetric

Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle.

Front Immunol

Center for Cancer Systems Biology and Department of Cancer Biology, Dana-Farber Cancer Institute, Boston, MA, United States.

Published: August 2020

The NF-κB transcription regulation system governs a diverse set of responses to various cytokine stimuli. With tools from biochemical characterizations, to omics-based whole genome investigations, great strides have been made in understanding how NF-κB transcription factors control the expression of specific sets of genes. Nonetheless, these efforts have also revealed a very large number of potential binding sites for NF-κB in the human genome, and a puzzle emerges when trying to explain how NF-κB selects from these many binding sites to direct cell-type- and stimulus-specific gene expression patterns. In this review, we surmise that target gene transcription can broadly be thought of as a function of the nuclear of the various NF-κB dimers, the of NF-κB dimers for the regulatory sequence and the of this regulatory site. We use this framework to place quantitative information that has been gathered about the NF-κB transcription regulation system into context and thus consider questions it answers, and questions it raises. We end with a brief discussion of some of the future prospects that new approaches could bring to our understanding of how NF-κB transcription factors orchestrate diverse responses in different biological contexts.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6450194PMC
http://dx.doi.org/10.3389/fimmu.2019.00609DOI Listing

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