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Quantitative Structure–Toxicity Relationship in Bioactive Molecules from a Conceptual DFT Perspective

Ranita Pal, Shanti G. Patra, Pratim Kumar Chattaraj

2022Pharmaceuticals18 citationsDOIOpen Access PDF

Abstract

The preclinical drug discovery stage often requires a large amount of costly and time-consuming experiments using huge sets of chemical compounds. In the last few decades, this process has undergone significant improvements by the introduction of quantitative structure-activity relationship (QSAR) modelling that uses a certain percentage of experimental data to predict the biological activity/property of compounds with similar structural skeleton and/or containing a particular functional group(s). The use of machine learning tools along with it has made life even easier for pharmaceutical researchers. Here, we discuss the toxicity of certain sets of bioactive compounds towards Pimephales promelas and Tetrahymena pyriformis in terms of the global conceptual density functional theory (CDFT)-based descriptor, electrophilicity index (ω). We have compared the results with those obtained by using the commonly used hydrophobicity parameter, logP (where P is the n-octanol/water partition coefficient), considering the greater ease of computing the ω descriptor. The Human African trypanosomiasis (HAT) curing activity of 32 pyridyl benzamide derivatives is also studied against Tryphanosoma brucei. In this review article, we summarize these multiple linear regression (MLR)-based QSAR studies in terms of electrophilicity (ω, ω2) and hydrophobicity (logP, (logP)2) parameters.

Topics & Concepts

Quantitative structure–activity relationshipMolecular descriptorPartition coefficientTetrahymena pyriformisDrug discoveryBiological systemChemistryComputer scienceComputational chemistryComputational biologyBiochemical engineeringStereochemistryBiologyOrganic chemistryBiochemistryEngineeringTetrahymenaComputational Drug Discovery MethodsSynthesis and biological activityFree Radicals and Antioxidants