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

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

The NF-κB transcription regulation system governs a diverse set of responses to various cytokine stimuli. With tools from in vitro biochemical characterizations, to omics-based whole genome investigations, great strides have been made in understanding how NF-κB transcription factors control the expr...

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Bibliographic Details
Main Authors: Ruth Brignall, Amy T. Moody, Shibin Mathew, Suzanne Gaudet
Format: Article
Language:English
Published: Frontiers Media S.A. 2019-03-01
Series:Frontiers in Immunology
Subjects:
NF-κB
transcription regulation
specificity
accessibility
competition
Online Access:https://www.frontiersin.org/article/10.3389/fimmu.2019.00609/full
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spelling doaj-cc57bd0eb3a944afbd836ac957ad188c2020-11-25T02:12:13ZengFrontiers Media S.A.Frontiers in Immunology1664-32242019-03-011010.3389/fimmu.2019.00609436564Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection PuzzleRuth Brignall0Ruth Brignall1Amy T. Moody2Amy T. Moody3Amy T. Moody4Amy T. Moody5Shibin Mathew6Shibin Mathew7Suzanne Gaudet8Suzanne Gaudet9Center for Cancer Systems Biology and Department of Cancer Biology, Dana-Farber Cancer Institute, Boston, MA, United StatesDepartment of Genetics, Harvard Medical School, Blavatnik Institute, Boston, MA, United StatesCenter for Cancer Systems Biology and Department of Cancer Biology, Dana-Farber Cancer Institute, Boston, MA, United StatesDepartment of Genetics, Harvard Medical School, Blavatnik Institute, Boston, MA, United StatesLaboratory for Systems Pharmacology, Harvard Medical School, Blavatnik Institute, Boston, MA, United StatesDepartment of Microbiology, Tufts University School of Medicine, Boston, MA, United StatesCenter for Cancer Systems Biology and Department of Cancer Biology, Dana-Farber Cancer Institute, Boston, MA, United StatesDepartment of Genetics, Harvard Medical School, Blavatnik Institute, Boston, MA, United StatesCenter for Cancer Systems Biology and Department of Cancer Biology, Dana-Farber Cancer Institute, Boston, MA, United StatesDepartment of Genetics, Harvard Medical School, Blavatnik Institute, Boston, MA, United StatesThe NF-κB transcription regulation system governs a diverse set of responses to various cytokine stimuli. With tools from in vitro 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 abundance of the various NF-κB dimers, the affinity of NF-κB dimers for the regulatory sequence and the availability 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.https://www.frontiersin.org/article/10.3389/fimmu.2019.00609/fullNF-κBtranscription regulationspecificityaccessibilitycompetition
collection DOAJ
language English
format Article
sources DOAJ
author Ruth Brignall
Ruth Brignall
Amy T. Moody
Amy T. Moody
Amy T. Moody
Amy T. Moody
Shibin Mathew
Shibin Mathew
Suzanne Gaudet
Suzanne Gaudet
spellingShingle Ruth Brignall
Ruth Brignall
Amy T. Moody
Amy T. Moody
Amy T. Moody
Amy T. Moody
Shibin Mathew
Shibin Mathew
Suzanne Gaudet
Suzanne Gaudet
Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle
Frontiers in Immunology
NF-κB
transcription regulation
specificity
accessibility
competition
author_facet Ruth Brignall
Ruth Brignall
Amy T. Moody
Amy T. Moody
Amy T. Moody
Amy T. Moody
Shibin Mathew
Shibin Mathew
Suzanne Gaudet
Suzanne Gaudet
author_sort Ruth Brignall
title Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle
title_short Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle
title_full Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle
title_fullStr Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle
title_full_unstemmed Considering Abundance, Affinity, and Binding Site Availability in the NF-κB Target Selection Puzzle
title_sort considering abundance, affinity, and binding site availability in the nf-κb target selection puzzle
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2019-03-01
description The NF-κB transcription regulation system governs a diverse set of responses to various cytokine stimuli. With tools from in vitro 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 abundance of the various NF-κB dimers, the affinity of NF-κB dimers for the regulatory sequence and the availability 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.
topic NF-κB
transcription regulation
specificity
accessibility
competition
url https://www.frontiersin.org/article/10.3389/fimmu.2019.00609/full
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