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Review

Multitasking models for quantitative structure–biological effect relationships: current status and future perspectives to speed up drug discovery

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Abstract

Introduction: Drug discovery is the process of designing new candidate medications for the treatment of diseases. Over many years, drugs have been identified serendipitously. Nowadays, chemoinformatics has emerged as a great ally, helping to rationalize drug discovery. In this sense, quantitative structure–activity relationships (QSAR) models have become complementary tools, permitting the efficient virtual screening for a diverse number of pharmacological profiles. Despite the applications of current QSAR models in the search for new drug candidates, many aspects remain unresolved. To date, classical QSAR models are able to predict only one type of biological effect (activity, toxicity, etc.) against only one type of generic target.

Areas covered: The present review discusses innovative and evolved QSAR models, which are focused on multitasking quantitative structure–biological effect relationships (mtk-QSBER). Such models can integrate multiple kinds of chemical and biological data, allowing the simultaneous prediction of pharmacological activities, toxicities and/or other safety profiles.

Expert opinion: The authors strongly believe, given the potential of mtk-QSBER models to simultaneously predict the dissimilar biological effects of chemicals, that they have much value as in silico tools for drug discovery. Indeed, these models can speed up the search for efficacious drugs in a number of areas, including fragment-based drug discovery and drug repurposing.

Acknowledgment

A Speck-Planche and MNDS Cordeiro contributed equally to this work.

Declaration of interest

The authors are supported by the Portuguese Fundação para a Ciência e a Tecnologia (FCT). MNDS Cordeiro is supported by Portuguese FCT grant No. Pest-C/EQB/LA0006/2011. A Speck-Planche has also received financial support given by the Portuguese FCT, QREN/POPH/MEC, and the European Social Fund (Grant. SFRH/BD/77690/2011). The authors have no other relevant affiliations or financial involvement with any organization or entity with a financial interest in or financial conflict with the subject matter or materials discussed in the manuscript apart from those disclosed.

Notes

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