An ensemble learning approach for modeling the systems biology of drug-induced injury

Joaquim Aguirre-Plans; Janet Piñero; Terezinha Souza; Giulia Callegaro; Steven J Kunnen; Ferran Sanz; Narcis Fernandez-Fuentes; Laura I Furlong; Emre Guney; Baldo Oliva

doi:10.1186/s13062-020-00288-x

An ensemble learning approach for modeling the systems biology of drug-induced injury

Biol Direct. 2021 Jan 12;16(1):5. doi: 10.1186/s13062-020-00288-x.

Authors

Affiliations

¹ Research Programme on Biomedical Informatics (GRIB), Hospital del Mar Medical Research Institute (IMIM), DCEXS, Pompeu Fabra University (UPF), Barcelona, Spain.
² Department of Toxicogenomics, Maastricht University, Maastricht, The Netherlands.
³ Leiden Academic Centre for Drug Research, Leiden University, Leiden, The Netherlands.
⁴ Department of Biosciences, U Science Tech, Universitat de Vic-Universitat Central de Catalunya, Vic, Spain.
⁵ Institute of Biological, Environmental and Rural Sciences, Aberystwyth University, Aberystwyth, UK.
⁶ Research Programme on Biomedical Informatics (GRIB), Hospital del Mar Medical Research Institute (IMIM), DCEXS, Pompeu Fabra University (UPF), Barcelona, Spain. baldo.oliva@upf.edu.

Abstract

Background: Drug-induced liver injury (DILI) is an adverse reaction caused by the intake of drugs of common use that produces liver damage. The impact of DILI is estimated to affect around 20 in 100,000 inhabitants worldwide each year. Despite being one of the main causes of liver failure, the pathophysiology and mechanisms of DILI are poorly understood. In the present study, we developed an ensemble learning approach based on different features (CMap gene expression, chemical structures, drug targets) to predict drugs that might cause DILI and gain a better understanding of the mechanisms linked to the adverse reaction.

Results: We searched for gene signatures in CMap gene expression data by using two approaches: phenotype-gene associations data from DisGeNET, and a non-parametric test comparing gene expression of DILI-Concern and No-DILI-Concern drugs (as per DILIrank definitions). The average accuracy of the classifiers in both approaches was 69%. We used chemical structures as features, obtaining an accuracy of 65%. The combination of both types of features produced an accuracy around 63%, but improved the independent hold-out test up to 67%. The use of drug-target associations as feature obtained the best accuracy (70%) in the independent hold-out test.

Conclusions: When using CMap gene expression data, searching for a specific gene signature among the landmark genes improves the quality of the classifiers, but it is still limited by the intrinsic noise of the dataset. When using chemical structures as a feature, the structural diversity of the known DILI-causing drugs hampers the prediction, which is a similar problem as for the use of gene expression information. The combination of both features did not improve the quality of the classifiers but increased the robustness as shown on independent hold-out tests. The use of drug-target associations as feature improved the prediction, specially the specificity, and the results were comparable to previous research studies.

Keywords: CAMDA; Cmap; Drug safety; Drug structure; Drug-induced liver injury; Hepatotoxicity; Machine learning; Systems biology.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Chemical and Drug Induced Liver Injury*
Drug-Related Side Effects and Adverse Reactions*
Humans
Machine Learning*
Models, Biological
Pharmaceutical Preparations / chemistry*
Systems Biology*

Substances

Pharmaceutical Preparations

Abstract

Publication types

MeSH terms

Substances

Grants and funding