Classification of toxicity effects of biotransformed hepatic drugs using whale optimized support vector machines

Alaa Tharwat; Yasmine S Moemen; Aboul Ella Hassanien

doi:10.1016/j.jbi.2017.03.002

Classification of toxicity effects of biotransformed hepatic drugs using whale optimized support vector machines

J Biomed Inform. 2017 Apr:68:132-149. doi: 10.1016/j.jbi.2017.03.002. Epub 2017 Mar 8.

Authors

Alaa Tharwat¹, Yasmine S Moemen², Aboul Ella Hassanien³

Affiliations

¹ Faculty of Engineering, Suez Canal University, Ismailia, Egypt; Scientific Research Group in Egypt (SRGE), Egypt(1).
² Scientific Research Group in Egypt (SRGE), Egypt(1); Clinical Pathology Department, National Liver Institute, Menoufia University, Egypt. Electronic address: yasmine_moemen@livereg.org.
³ Scientific Research Group in Egypt (SRGE), Egypt(1); Faculty of Computers and Information, Cairo University, Egypt. Electronic address: aboitcairo@gmail.com.

PMID: 28286029
DOI: 10.1016/j.jbi.2017.03.002

Abstract

Measuring toxicity is an important step in drug development. Nevertheless, the current experimental methods used to estimate the drug toxicity are expensive and time-consuming, indicating that they are not suitable for large-scale evaluation of drug toxicity in the early stage of drug development. Hence, there is a high demand to develop computational models that can predict the drug toxicity risks. In this study, we used a dataset that consists of 553 drugs that biotransformed in liver. The toxic effects were calculated for the current data, namely, mutagenic, tumorigenic, irritant and reproductive effect. Each drug is represented by 31 chemical descriptors (features). The proposed model consists of three phases. In the first phase, the most discriminative subset of features is selected using rough set-based methods to reduce the classification time while improving the classification performance. In the second phase, different sampling methods such as Random Under-Sampling, Random Over-Sampling and Synthetic Minority Oversampling Technique (SMOTE), BorderLine SMOTE and Safe Level SMOTE are used to solve the problem of imbalanced dataset. In the third phase, the Support Vector Machines (SVM) classifier is used to classify an unknown drug into toxic or non-toxic. SVM parameters such as the penalty parameter and kernel parameter have a great impact on the classification accuracy of the model. In this paper, Whale Optimization Algorithm (WOA) has been proposed to optimize the parameters of SVM, so that the classification error can be reduced. The experimental results proved that the proposed model achieved high sensitivity to all toxic effects. Overall, the high sensitivity of the WOA+SVM model indicates that it could be used for the prediction of drug toxicity in the early stage of drug development.

Keywords: Imbalanced dataset; Random sampling; Support Vector Machines (SVM); Synthetic Minority Over-sampling Technique (SMOTE); Toxic effects; Whale Optimization Algorithm (WOA).

MeSH terms

Algorithms
Chemical and Drug Induced Liver Injury
Drug Discovery
Drug-Related Side Effects and Adverse Reactions*
Forecasting
Humans
Support Vector Machine*