Pharmacophore Fingerprinting. 1. Application to QSAR and Focused Library Design

McGregor, Malcolm J.; Muskal, Steven M.

doi:10.1021/ci980159j

Cited by 167 publications

(150 citation statements)

References 27 publications

(45 reference statements)

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“…There are very few methods for modeling data using multiple pharmacophores (Chen et al, 1999;McGregor and Muskal, 1999;Penzotti et al, 2002). The method described here is based around the use of clustering and a genetic algorithm to select a small number of relevant and diverse pharmacophores from a pharmacophore fingerprint.…”

Section: Discussionmentioning

confidence: 99%

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Multiple Pharmacophores for the Investigation of Human UDP-Glucuronosyltransferase Isoform Substrate Selectivity

Sorich¹,

Miners²,

McKinnon³

et al. 2004

Mol Pharmacol

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The UDP-glucuronosyltransferase (UGT) enzyme 'superfamily' contributes to the metabolism of a myriad of drugs, nondrug xenobiotic agents, and endogenous compounds. Although the individual UGT isoforms exhibit distinct but overlapping substrate selectivities, structural features of substrates that confer selectivity remain largely unknown. Using methods developed for pharmacophore fingerprinting combined with optimization and pattern recognition techniques, subsets of pharmacophores associated with the substrates and nonsubstrates of 12 human UGT isoforms were selected to generate predictive models of substrate selectivity and to elucidate the chemical and structural features associated with substrates and nonsubstrates. For all 12 UGT isoforms, the pharmacophore model generated showed predictive ability, as determined by a test set comprising 30% of the available data for each isoform.Models for UGT1A6, -1A7, -1A9, and -2B4 displayed the best predictive ability (Ͼ75% of test set predicted correctly) and were further analyzed to interpret the pharmacophores selected as important. The individual pharmacophores differed among isoforms but generally represented relatively simple structural and chemical features. For example, an aromatic ring attached to the nucleophilic group was found to increase the likelihood of glucuronidation by UGT1A6, UGT1A7 and UGT1A9. A large hydrophobic region close to the nucleophile and a hydrogen bond acceptor 10 Å from the nucleophile were found to be common to most UGT2B4 substrates. The pharmacophores further suggest that the environment immediately adjacent to the nucleophilic site of conjugation is an important determinant of metabolism by a particular UGT.

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Section: Discussionmentioning

confidence: 99%

“…Thus, at least for some isoforms, multiple pharmacophores may be required to model metabolism by UGT. Although algorithms for multiple pharmacophore perception exist (Chen et al, 1999;McGregor and Muskal, 1999;Penzotti et al, 2002), they are generally used for chemical database searching rather than accurate prediction of chemical properties.…”

mentioning

confidence: 99%

Multiple Pharmacophores for the Investigation of Human UDP-Glucuronosyltransferase Isoform Substrate Selectivity

Sorich¹,

Miners²,

McKinnon³

et al. 2004

Mol Pharmacol

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“…All these approaches have variety of applications in drug research concerning to the characterization of chemical structures, diversity/ similarity analysis, selection and acquisition of compound from libraries and databases [110][111][112][113][114]. Hologram QSAR (HQSAR), a QSAR technique devoid of molecular descriptors, also uses characteristic fragment fingerprints (molecular holograms) as predictive variables of biological activity [115].…”

Section: Molecular Fingerprintsmentioning

confidence: 99%

Chemical Structure Indices in In Silico Molecular Design

Prabhakar

2008

Sci Pharm

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“…However, this assumption clearly does not hold for many drug-metabolising enzymes, which often generate multiple metabolites from a single chemical presumably due to multiple binding modes. While the field of drug-metabolism prediction is a novel application for such 'pharmacophore fingerprints', successful application of this concept has been reported in other fields of drug discovery [54,55]. Indeed multiple pharmacophores have also been utilised to characterise molecular recognition by a number of xenobiotic binding proteins [56][57][58].…”

Section: Classificationmentioning

confidence: 99%

Towards integrated ADME prediction: past, present and future directions for modelling metabolism by UDP-glucuronosyltransferases

Smith

Sorich

Low

et al. 2004

Journal of Molecular Graphics and Modelling

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Undesirable absorption, distribution, metabolism, excretion (ADME) properties are the cause of many drug development failures and this has led to the need to identify such problems earlier in the development process. This review highlights computational (in silico) approaches that have been used to identify the characteristics of ligands influencing molecular recognition and/or metabolism by the drug-metabolising enzyme UDP-gucuronosyltransferase (UGT). Current studies applying pharmacophore elucidation, 2D-quantitative structure metabolism relationships (2D-QSMR), 3D-quantitative structure metabolism relationships (3D-QSMR), and non-linear pattern recognition techniques such as artificial neural networks and support vector machines for modelling metabolism by UGT are reported. An assessment of the utility of in silico approaches for the qualitative and quantitative prediction of drug glucuronidation parameters highlights the benefit of using multiple pharmacophores and also non-linear techniques for classification. Some of the challenges facing the development of generalisable models for predicting metabolism by UGT, including the need for screening of more diverse structures, are also outlined.

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Pharmacophore Fingerprinting. 1. Application to QSAR and Focused Library Design

Cited by 167 publications

References 27 publications

Multiple Pharmacophores for the Investigation of Human UDP-Glucuronosyltransferase Isoform Substrate Selectivity

Multiple Pharmacophores for the Investigation of Human UDP-Glucuronosyltransferase Isoform Substrate Selectivity

Chemical Structure Indices in In Silico Molecular Design

Towards integrated ADME prediction: past, present and future directions for modelling metabolism by UDP-glucuronosyltransferases

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