Optimization of the TeraTox Assay for Preclinical Teratogenicity Assessment

Author:

Jaklin Manuela12ORCID,Zhang Jitao David1ORCID,Schäfer Nicole1,Clemann Nicole1,Barrow Paul1,Küng Erich1,Sach-Peltason Lisa1,McGinnis Claudia3,Leist Marcel2ORCID,Kustermann Stefan1

Affiliation:

1. Pharmaceutical Sciences, Pharma Research and Early Development, Roche Innovation Center Basel, F. Hoffmann-La Roche Ltd, 4070 Basel, Switzerland

2. Department for In Vitro Toxicology and Biomedicine Inaugurated by the Doerenkamp-Zbinden Foundation, University of Konstanz, 78464 Konstanz, Germany

3. Drug Discovery Unit, University of Dundee, DD1 5EH Dundee, UK

Abstract

Abstract Current animal-free methods to assess teratogenicity of drugs under development still deliver high numbers of false negatives. To improve the sensitivity of human teratogenicity prediction, we characterized the TeraTox test, a newly developed multilineage differentiation assay using 3D human-induced pluripotent stem cells. TeraTox produces primary output concentration-dependent cytotoxicity and altered gene expression induced by each test compound. These data are fed into an interpretable machine-learning model to perform prediction, which relates to the concentration-dependent human teratogenicity potential of drug candidates. We applied TeraTox to profile 33 approved pharmaceuticals and 12 proprietary drug candidates with known in vivo data. Comparing TeraTox predictions with known human or animal toxicity, we report an accuracy of 69% (specificity: 53%, sensitivity: 79%). TeraTox performed better than 2 quantitative structure-activity relationship models and had a higher sensitivity than the murine embryonic stem cell test (accuracy: 58%, specificity: 76%, and sensitivity: 46%) run in the same laboratory. The overall prediction accuracy could be further improved by combining TeraTox and mouse embryonic stem cell test results. Furthermore, patterns of altered gene expression revealed by TeraTox may help grouping toxicologically similar compounds and possibly deducing common modes of action. The TeraTox assay and the dataset described here therefore represent a new tool and a valuable resource for drug teratogenicity assessment.

Funder

CEFIC

European Chemical Industry Council

BMBF

Bundesministerium für Bildung und Forschung

European Food Safety Authority

Danish Environmental Protection Agency

European Union’s Horizon 2020

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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