GenomeCAT: a versatile tool for the analysis and integrative visualization of DNA copy number variants

Katrin Tebel; Vivien Boldt; Anne Steininger; Matthias Port; Grit Ebert; Reinhard Ullmann

doi:10.1186/s12859-016-1430-x

GenomeCAT: a versatile tool for the analysis and integrative visualization of DNA copy number variants

BMC Bioinformatics. 2017 Jan 6;18(1):19. doi: 10.1186/s12859-016-1430-x.

Authors

Katrin Tebel¹, Vivien Boldt^{1

2}, Anne Steininger^{1

2}, Matthias Port³, Grit Ebert^{1

2}, Reinhard Ullmann^{4

5}

Affiliations

¹ Max Planck Institute for Molecular Genetics, 14195, Berlin, Germany.
² Department of Biology, Chemistry and Pharmacy, Free University Berlin, 14195, Berlin, Germany.
³ Institut für Radiobiologie der Bundeswehr in Verb. mit der Universität Ulm, 80937, Munich, Germany.
⁴ Max Planck Institute for Molecular Genetics, 14195, Berlin, Germany. reinhard1ullmann@bundeswehr.org.
⁵ Institut für Radiobiologie der Bundeswehr in Verb. mit der Universität Ulm, 80937, Munich, Germany. reinhard1ullmann@bundeswehr.org.

Abstract

Background: The analysis of DNA copy number variants (CNV) has increasing impact in the field of genetic diagnostics and research. However, the interpretation of CNV data derived from high resolution array CGH or NGS platforms is complicated by the considerable variability of the human genome. Therefore, tools for multidimensional data analysis and comparison of patient cohorts are needed to assist in the discrimination of clinically relevant CNVs from others.

Results: We developed GenomeCAT, a standalone Java application for the analysis and integrative visualization of CNVs. GenomeCAT is composed of three modules dedicated to the inspection of single cases, comparative analysis of multidimensional data and group comparisons aiming at the identification of recurrent aberrations in patients sharing the same phenotype, respectively. Its flexible import options ease the comparative analysis of own results derived from microarray or NGS platforms with data from literature or public depositories. Multidimensional data obtained from different experiment types can be merged into a common data matrix to enable common visualization and analysis. All results are stored in the integrated MySQL database, but can also be exported as tab delimited files for further statistical calculations in external programs.

Conclusions: GenomeCAT offers a broad spectrum of visualization and analysis tools that assist in the evaluation of CNVs in the context of other experiment data and annotations. The use of GenomeCAT does not require any specialized computer skills. The various R packages implemented for data analysis are fully integrated into GenomeCATs graphical user interface and the installation process is supported by a wizard. The flexibility in terms of data import and export in combination with the ability to create a common data matrix makes the program also well suited as an interface between genomic data from heterogeneous sources and external software tools. Due to the modular architecture the functionality of GenomeCAT can be easily extended by further R packages or customized plug-ins to meet future requirements.

Keywords: DNA copy number variants; Integrative visualization; Microarray; NGS.

MeSH terms

Computer Simulation
DNA Copy Number Variations*
Genome, Human
Genomics
Humans
Models, Theoretical
Reproducibility of Results
Software*