Multi-omics HeCaToS dataset of repeated dose toxicity for cardiotoxic & hepatotoxic compounds
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Published:2022-11-14
Issue:1
Volume:9
Page:
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ISSN:2052-4463
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Container-title:Scientific Data
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language:en
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Short-container-title:Sci Data
Author:
Verheijen Marcha, Sarkans UgisORCID, Wolski Witold, Jennen Danyel, Caiment Florian, Kleinjans Jos, Agarkova Irina, Atkinson Francis L., Bachmann Ivo, Baier Vanessa, Barel Gal, Bauer Chris, van den Beucken Twan, Boerno Stefan, Bosc Nicolas, Carey Conn, Castell José V., Clayton Olivia, Cordes Henrik, Deeb Sally, Gmuender Hans, Gotta Stefano, Guye Patrick, Hersey Anne, Herwig Ralf, Heymans Stephane, Hunt Peter, Hunter Fiona M. I., Hynes James, Keun Hector, Kouloura Eirini, Kuepfer Lars, Kunz Laura, Lewalle Alex, Lienhard Matthias, Martínez-Sena Teresa, Merken Jort, Minguet Jasmine, Nguyen Nhan, Niederer Steven, Nudischer Ramona, Asensio Juan Ochoteco, Oliveira Bernardo, Panse Christian, Pluess Carla, Roth Adrian B., Schlapbach Ralph, Schrooders Yannick, Schuchhardt Johannes, Segall Matthew, Selevsek Nathalie, Sepulveda Pilar, Smit Ines, Thiel Christoph, Timmermann Bernd, Wittenberger Timo, Zerck Alexandra,
Abstract
AbstractThe data currently described was generated within the EU/FP7 HeCaToS project (Hepatic and Cardiac Toxicity Systems modeling). The project aimed to develop an in silico prediction system to contribute to drug safety assessment for humans. For this purpose, multi-omics data of repeated dose toxicity were obtained for 10 hepatotoxic and 10 cardiotoxic compounds. Most data were gained from in vitro experiments in which 3D microtissues (either hepatic or cardiac) were exposed to a therapeutic (physiologically relevant concentrations calculated through PBPK-modeling) or a toxic dosing profile (IC20 after 7 days). Exposures lasted for 14 days and samples were obtained at 7 time points (therapeutic doses: 2-8-24-72-168-240-336 h; toxic doses 0-2-8-24-72-168-240 h). Transcriptomics (RNA sequencing & microRNA sequencing), proteomics (LC-MS), epigenomics (MeDIP sequencing) and metabolomics (LC-MS & NMR) data were obtained from these samples. Furthermore, functional endpoints (ATP content, Caspase3/7 and O2 consumption) were measured in exposed microtissues. Additionally, multi-omics data from human biopsies from patients are available. This data is now being released to the scientific community through the BioStudies data repository (https://www.ebi.ac.uk/biostudies/).
Funder
VSNU Vereniging van Universiteiten European Commission 7th Framework Program with the project HeCaToS
Publisher
Springer Science and Business Media LLC
Subject
Library and Information Sciences,Statistics, Probability and Uncertainty,Computer Science Applications,Education,Information Systems,Statistics and Probability
Cited by
5 articles.
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