4.6 Article

Screening drug effects in patient-derived cancer cells links organoid responses to genome alterations

Journal

MOLECULAR SYSTEMS BIOLOGY
Volume 13, Issue 11, Pages -

Publisher

WILEY
DOI: 10.15252/msb.20177697

Keywords

cancer organoids; confocal microscopy; high-throughput screening; personalized drug screen; pharmacogenomics

Funding

  1. Annemarie Poustka fellowship of the German Cancer Research Center
  2. BMBF-Heidelberg Center for Human Bioinformatics (HD-HuB) within the German Network for Bioinformatics Infrastructure (de.NBI) [031A537A, 031A537C]
  3. Helmholtz International Graduate School for Cancer Research
  4. DKFZ NCT3.0 Precision Oncology Program PANC-STRAT [NCT3.0_2015.16 PDAC POP]
  5. BMBF-e:Med program for systems medicine (PANC-STRAT) [01ZX1305]
  6. Dietmar Hopp Foundation
  7. Swiss Bridge Foundation and iMed Program (Helmholtz Association)
  8. DKFZ-HIPO [HIPO 059]

Ask authors/readers for more resources

Cancer drug screening in patient-derived cells holds great promise for personalized oncology and drug discovery but lacks standardization. Whether cells are cultured as conventional monolayer or advanced, matrix-dependent organoid cultures influences drug effects and thereby drug selection and clinical success. To precisely compare drug profiles in differently cultured primary cells, we developed DeathPro, an automated microscopy-based assay to resolve drug-induced cell death and proliferation inhibition. Using DeathPro, we screened cells from ovarian cancer patients in monolayer or organoid culture with clinically relevant drugs. Druginduced growth arrest and efficacy of cytostatic drugs differed between the two culture systems. Interestingly, drug effects in organoids were more diverse and had lower therapeutic potential. Genomic analysis revealed novel links between drug sensitivity and DNA repair deficiency in organoids that were undetectable in monolayers. Thus, our results highlight the dependency of cytostatic drugs and pharmacogenomic associations on culture systems, and guide culture selection for drug tests.

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