Decoding mechanism of action and sensitivity to drug candidates from integrated transcriptome and chromatin state.

Carraro, Caterina; Aschenbrenner, Anna Christin; Schulte-Schrepping, Jonas; Mukherjee, Sach; Gandin, Valentina; Oestreich, Marie; Horne, Arik; Bonaguro, Lorenzo; Schultze, Joachim L; Ulas, Thomas; Gatto, Barbara; Helbing, Tim; Warnat-Herresthal, Stefanie; Händler, Kristian; De Franco, Michele; Goettlich, Richard

doi:10.7554/eLife.78012

Journal Article

DZNE-2022-01569

Decoding mechanism of action and sensitivity to drug candidates from integrated transcriptome and chromatin state.

Carraro, C.Extern* ; Bonaguro, L.DZNE* ; Schulte-Schrepping, J.DZNE* ; Horne, A.DZNE* ; Oestreich, M.DZNE* ; Warnat-Herresthal, S.DZNE* ; Helbing, T. ; De Franco, M. ; Händler, K.DZNE* ; Mukherjee, S.DZNE* ; Ulas, T.DZNE* ; Gandin, V. ; Goettlich, R. ; Aschenbrenner, A. C.DZNE* ; Schultze, J. L.DZNE* ; Gatto, B.

2022
eLife Sciences Publications Cambridge

eLife 11, e78012 (2022) [10.7554/eLife.78012]

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Please use a persistent id in citations: doi:10.7554/eLife.78012

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.

Keyword(s): Chromatin (MeSH) ; Precision Medicine (MeSH) ; RNA (MeSH) ; Transcriptome (MeSH) ; Transposases: metabolism (MeSH) ; chromatin accessibility ; computational biology ; drug candidate ; human ; mechanism of action ; multi-omics ; sensitivity ML prediction ; systems biology ; transcriptome ; Chromatin ; RNA ; Transposases

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ddc:600

Note: CC BY: https://creativecommons.org/licenses/by/4.0/

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Appears in the scientific report 2022

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Institute Collections > BN DZNE > BN DZNE-R&D PRECISE
Document types > Articles > Journal Article
Institute Collections > BN DZNE > BN DZNE-AG Mukherjee
Institute Collections > BN DZNE > BN DZNE-PRECISE
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Record created 2022-10-11, last modified 2023-09-15

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