Database Commons
Database Commons

a catalog of worldwide biological databases

Database Profile

Cistrome Data Browser

General information

URL: http://db3.cistrome.org/browser
Full name: Cistrome Data Browser
Description: Cistrome Data Browser v3.0 is a resource for ChIP-seq, ATAC-seq, and DNase-seq data from humans and mice, providing maps of genome-wide locations of transcription factors, cofactors, chromatin remodelers, histone modifications, and accessible chromatin regions. It contains approximately 45,000 human and 44,000 mouse samples, with 32,000 new datasets added.
Year founded: 2023
Last update: 2023-11-16
Version: v3.0
Accessibility:
Accessible
Country/Region: United States

Classification & Tag

Data type:
DNA
Data object:
Database category:
Major species:
Keywords:

Contact information

University/Institution: Dana-Farber Cancer Institute
Address: Department of Data Science, Dana-Farber Cancer Institute, Boston, MA, USA
City: Boston
Province/State: Massachusetts
Country/Region: United States
Contact name (PI/Team): Clifford A Meyer
Contact email (PI/Helpdesk): cliff_meyer@ds.dfci.harvard.edu

Publications

37971305
Cistrome Data Browser: integrated search, analysis and visualization of chromatin data. [PMID: 37971305]
Len Taing, Ariaki Dandawate, Sehi L'Yi, Nils Gehlenborg, Myles Brown, Clifford A Meyer

The Cistrome Data Browser is a resource of ChIP-seq, ATAC-seq and DNase-seq data from humans and mice. It provides maps of the genome-wide locations of transcription factors, cofactors, chromatin remodelers, histone post-translational modifications and regions of chromatin accessible to endonuclease activity. Cistrome DB v3.0 contains approximately 45 000 human and 44 000 mouse samples with about 32 000 newly collected datasets compared to the previous release. The Cistrome DB v3.0 user interface is implemented as a single page application that unifies menu driven and data driven search functions and provides an embedded genome browser, which allows users to find and visualize data more effectively. Users can find informative chromatin profiles through keyword, menu, and data-driven search tools. Browser search functions can predict the regulators of query genes as well as the cell type and factor dependent functionality of potential cis-regulatory elements. Cistrome DB v3.0 expands the display of quality control statistics, incorporates sequence logos into motif enrichment displays and includes more expansive sample metadata. Cistrome DB v3.0 is available at http://db3.cistrome.org/browser.

Nucleic Acids Res. 2024:52(D1) | 34 Citations (from Europe PMC, 2025-12-13)
30462313
Cistrome Data Browser: expanded datasets and new tools for gene regulatory analysis. [PMID: 30462313]
Zheng R, Wan C, Mei S, Qin Q, Wu Q, Sun H, Chen CH, Brown M, Zhang X, Meyer CA, Liu XS.

The Cistrome Data Browser (DB) is a resource of human and mouse cis-regulatory information derived from ChIP-seq, DNase-seq and ATAC-seq chromatin profiling assays, which map the genome-wide locations of transcription factor binding sites, histone post-translational modifications and regions of chromatin accessible to endonuclease activity. Currently, the Cistrome DB contains approximately 47,000 human and mouse samples with about 24,000 newly collected datasets compared to the previous release two years ago. Furthermore, the Cistrome DB has a new Toolkit module with several features that allow users to better utilize the large-scale ChIP-seq, DNase-seq, and ATAC-seq data. First, users can query the factors which are likely to regulate a specific gene of interest. Second, the Cistrome DB Toolkit facilitates searches for factor binding, histone modifications, and chromatin accessibility in any given genomic interval shorter than 2Mb. Third, the Toolkit can determine the most similar ChIP-seq, DNase-seq, and ATAC-seq samples in terms of genomic interval overlaps with user-provided genomic interval sets. The Cistrome DB is a user-friendly, up-to-date, and well maintained resource, and the new tools will greatly benefit the biomedical research community. The database is freely available at http://cistrome.org/db, and the Toolkit is at http://dbtoolkit.cistrome.org.

Nucleic Acids Res. 2019:47(D1) | 627 Citations (from Europe PMC, 2025-12-13)
27789702
Cistrome Data Browser: a data portal for ChIP-Seq and chromatin accessibility data in human and mouse. [PMID: 27789702]
Mei S, Qin Q, Wu Q, Sun H, Zheng R, Zang C, Zhu M, Wu J, Shi X, Taing L, Liu T, Brown M, Meyer CA, Liu XS.

Chromatin immunoprecipitation, DNase I hypersensitivity and transposase-accessibility assays combined with high-throughput sequencing enable the genome-wide study of chromatin dynamics, transcription factor binding and gene regulation. Although rapidly accumulating publicly available ChIP-seq, DNase-seq and ATAC-seq data are a valuable resource for the systematic investigation of gene regulation processes, a lack of standardized curation, quality control and analysis procedures have hindered extensive reuse of these data. To overcome this challenge, we built the Cistrome database, a collection of ChIP-seq and chromatin accessibility data (DNase-seq and ATAC-seq) published before January 1, 2016, including 13 366 human and 9953 mouse samples. All the data have been carefully curated and processed with a streamlined analysis pipeline and evaluated with comprehensive quality control metrics. We have also created a user-friendly web server for data query, exploration and visualization. The resulting Cistrome DB (Cistrome Data Browser), available online at http://cistrome.org/db, is expected to become a valuable resource for transcriptional and epigenetic regulation studies. © The Author(s) 2016. Published by Oxford University Press on behalf of Nucleic Acids Research.

Nucleic Acids Res. 2017:45(D1) | 434 Citations (from Europe PMC, 2025-12-13)

Ranking

All databases:
129/6895 (98.144%)
Gene genome and annotation:
50/2021 (97.575%)
Interaction:
21/1194 (98.325%)
129
Total Rank
1,035
Citations
129.375
z-index

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Record metadata

Created on: 2024-07-15
Curated by:
Shiting Wang [2024-08-30]
Shiting Wang [2024-08-29]
Miaomiao Wang [2024-07-18]
zheng luo [2024-07-15]