| Literature DB >> 36043458 |
Caterina Carraro1, Lorenzo Bonaguro2,3, Jonas Schulte-Schrepping2,3, Arik Horne2,3, Marie Oestreich2, Stefanie Warnat-Herresthal2,3, Tim Helbing4, Michele De Franco1, Kristian Haendler2,5,6, Sach Mukherjee7,8, Thomas Ulas2,3,5, Valentina Gandin1, Richard Goettlich4, Anna C Aschenbrenner2,3,5,9, Joachim L Schultze2,3,5, Barbara Gatto1.
Abstract
Omics-based technologies are driving major advances in precision medicine, but efforts are still required to consolidate their use in drug discovery. In this work, we exemplify the use of multi-omics to support the development of 3-chloropiperidines, a new class of candidate anticancer agents. Combined analyses of transcriptome and chromatin accessibility elucidated the mechanisms underlying sensitivity to test agents. Furthermore, we implemented a new versatile strategy for the integration of RNA- and ATAC-seq (Assay for Transposase-Accessible Chromatin) data, able to accelerate and extend the standalone analyses of distinct omic layers. This platform guided the construction of a perturbation-informed basal signature predicting cancer cell lines' sensitivity and to further direct compound development against specific tumor types. Overall, this approach offers a scalable pipeline to support the early phases of drug discovery, understanding of mechanisms, and potentially inform the positioning of therapeutics in the clinic.Entities:
Keywords: chromatin accessibility; computational biology; drug candidate; human; mechanism of action; multi-omics; sensitivity ML prediction; systems biology; transcriptome
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Year: 2022 PMID: 36043458 PMCID: PMC9433094 DOI: 10.7554/eLife.78012
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.713