ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them

ChIP-seq reveals genomic regions where proteins, e.g. transcription factors (TFs) interact with DNA. A substantial fraction of these regions, however, do not contain the cognate binding site for the TF of interest. This phenomenon might be explained by protein–protein interactions and co-precipitati...

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Autores principales: Czipa, Erik, Schiller, Mátyás, Nagy, Tibor, Kontra, Levente, Steiner, László, Koller, Júlia, Pálné-Szén, Orsolya, Barta, Endre
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2020
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6964213/
https://www.ncbi.nlm.nih.gov/pubmed/31942977
http://dx.doi.org/10.1093/database/baz141
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author Czipa, Erik
Schiller, Mátyás
Nagy, Tibor
Kontra, Levente
Steiner, László
Koller, Júlia
Pálné-Szén, Orsolya
Barta, Endre
author_facet Czipa, Erik
Schiller, Mátyás
Nagy, Tibor
Kontra, Levente
Steiner, László
Koller, Júlia
Pálné-Szén, Orsolya
Barta, Endre
author_sort Czipa, Erik
collection PubMed
description ChIP-seq reveals genomic regions where proteins, e.g. transcription factors (TFs) interact with DNA. A substantial fraction of these regions, however, do not contain the cognate binding site for the TF of interest. This phenomenon might be explained by protein–protein interactions and co-precipitation of interacting gene regulatory elements. We uniformly processed 3727 human ChIP-seq data sets and determined the cistrome of 292 TFs, as well as the distances between the TF binding motif centers and the ChIP-seq peak summits. ChIPSummitDB enables the analysis of ChIP-seq data using multiple approaches. The 292 cistromes and corresponding ChIP-seq peak sets can be browsed in GenomeView. Overlapping SNPs can be inspected in dbSNPView. Most importantly, the MotifView and PairShiftView pages show the average distance between motif centers and overlapping ChIP-seq peak summits and distance distributions thereof, respectively. In addition to providing a comprehensive human TF binding site collection, the ChIPSummitDB database and web interface allows for the examination of the topological arrangement of TF complexes genome-wide. ChIPSummitDB is freely accessible at http://summit.med.unideb.hu/summitdb/. The database will be regularly updated and extended with the newly available human and mouse ChIP-seq data sets.
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spelling pubmed-69642132020-01-24 ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them Czipa, Erik Schiller, Mátyás Nagy, Tibor Kontra, Levente Steiner, László Koller, Júlia Pálné-Szén, Orsolya Barta, Endre Database (Oxford) Original Article ChIP-seq reveals genomic regions where proteins, e.g. transcription factors (TFs) interact with DNA. A substantial fraction of these regions, however, do not contain the cognate binding site for the TF of interest. This phenomenon might be explained by protein–protein interactions and co-precipitation of interacting gene regulatory elements. We uniformly processed 3727 human ChIP-seq data sets and determined the cistrome of 292 TFs, as well as the distances between the TF binding motif centers and the ChIP-seq peak summits. ChIPSummitDB enables the analysis of ChIP-seq data using multiple approaches. The 292 cistromes and corresponding ChIP-seq peak sets can be browsed in GenomeView. Overlapping SNPs can be inspected in dbSNPView. Most importantly, the MotifView and PairShiftView pages show the average distance between motif centers and overlapping ChIP-seq peak summits and distance distributions thereof, respectively. In addition to providing a comprehensive human TF binding site collection, the ChIPSummitDB database and web interface allows for the examination of the topological arrangement of TF complexes genome-wide. ChIPSummitDB is freely accessible at http://summit.med.unideb.hu/summitdb/. The database will be regularly updated and extended with the newly available human and mouse ChIP-seq data sets. Oxford University Press 2020-01-14 /pmc/articles/PMC6964213/ /pubmed/31942977 http://dx.doi.org/10.1093/database/baz141 Text en © The Author(s) 2020. Published by Oxford University Press. http://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Czipa, Erik
Schiller, Mátyás
Nagy, Tibor
Kontra, Levente
Steiner, László
Koller, Júlia
Pálné-Szén, Orsolya
Barta, Endre
ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
title ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
title_full ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
title_fullStr ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
title_full_unstemmed ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
title_short ChIPSummitDB: a ChIP-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
title_sort chipsummitdb: a chip-seq-based database of human transcription factor binding sites and the topological arrangements of the proteins bound to them
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6964213/
https://www.ncbi.nlm.nih.gov/pubmed/31942977
http://dx.doi.org/10.1093/database/baz141
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