Comparison of Zebrafish Larvae and hiPSC Cardiomyocytes for Predicting Drug-Induced Cardiotoxicity in Humans

Author:

Dyballa Sylvia1,Miñana Rafael1,Rubio-Brotons Maria1,Cornet Carles1,Pederzani Tiziana1,Escaramis Georgia234,Garcia-Serna Ricard5,Mestres Jordi567,Terriente Javier1ORCID

Affiliation:

1. ZeClinics SL, IGTP (German Trias and Pujol Institute), Badalona 08916, Spain

2. CIBER Epidemiology and Public Health

3. Department of Biomedicine, Faculty of Life Science and Health, University of Barcelona 08036, Barcelona, Spain

4. Research Group on Statistics, Econometrics and Health (GRECS), UdG, Girona 17071, Spain

5. Chemotargets SL, Parc Científic de Barcelona, Barcelona 08028, Spain

6. Systems Pharmacology, Research Program on Biomedical Informatics (GRIB), IMIM Hospital del Mar Medical Research Institute, Barcelona 08002, Spain

7. University Pompeu Fabra, PRBB (Barcelona Biomedical Research Park), Barcelona 08002, Spain

Abstract

Abstract Cardiovascular drug toxicity is responsible for 17% of drug withdrawals in clinical phases, half of post-marketed drug withdrawals and remains an important adverse effect of several marketed drugs. Early assessment of drug-induced cardiovascular toxicity is mandatory and typically done in cellular systems and mammals. Current in vitro screening methods allow high-throughput but are biologically reductionist. The use of mammal models, which allow a better translatability for predicting clinical outputs, is low-throughput, highly expensive, and ethically controversial. Given the analogies between the human and the zebrafish cardiovascular systems, we propose the use of zebrafish larvae during early drug discovery phases as a balanced model between biological translatability and screening throughput for addressing potential liabilities. To this end, we have developed a high-throughput screening platform that enables fully automatized in vivo image acquisition and analysis to extract a plethora of relevant cardiovascular parameters: heart rate, arrhythmia, AV blockage, ejection fraction, and blood flow, among others. We have used this platform to address the predictive power of zebrafish larvae for detecting potential cardiovascular liabilities in humans. We tested a chemical library of 92 compounds with known clinical cardiotoxicity profiles. The cross-comparison with clinical data and data acquired from human induced pluripotent stem cell cardiomyocytes calcium imaging showed that zebrafish larvae allow a more reliable prediction of cardiotoxicity than cellular systems. Interestingly, our analysis with zebrafish yields similar predictive performance as previous validation meta-studies performed with dogs, the standard regulatory preclinical model for predicting cardiotoxic liabilities prior to clinical phases.

Funder

European Union’s Horizon 2020

MINECO

EMPLEA

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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