Comparative Molecular Field Analysis of substrates for an Aryl sulfotransferase based on catalytic mechanism and protein homology modeling

Vyas Sharma; Michael W Duffel

doi:10.1021/jm010481c

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Comparative Molecular Field Analysis of substrates for an Aryl sulfotransferase based on catalytic mechanism and protein homology modeling

Journal article

Peer reviewed

Comparative Molecular Field Analysis of substrates for an Aryl sulfotransferase based on catalytic mechanism and protein homology modeling

Vyas Sharma and Michael W Duffel

Journal of medicinal chemistry, Vol.45(25), pp.5514-5522

2002

DOI: 10.1021/jm010481c

PMID: 12459019

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Abstract

Comparative Molecular Field Analysis (CoMFA) methods were used to produce a 3D-QSAR model that correlated the catalytic efficiency of rat hepatic aryl sulfotransferase (AST) IV, expressed as log(kcat/Km), with the molecular structures of its substrates. A total of 35 substrate molecules were used to construct a CoMFA model that was evaluated on the basis of its leave-one-out cross-validated partial least-squares value (q2) and its ability to predict the activity of six additional substrates not used in the training set. The model was constructed using substrate conformations that favored (1) proton abstraction by the catalytic histidine residue, (2) an inline sulfuryl-group transfer mechanism, and (3) constraints imposed by the residues lining the substrate binding pocket of a homology model of AST IV. This CoMFA model had a q2 value of 0.691, and it successfully predicted the activities of the six molecules not used in the training set. A final CoMFA model was constructed using the same methodology but with molecules from both the training set and the test set. Its q2 value was 0.701, and it had a non-cross-validated r2 value of 0.922. The contour coefficient map generated by this CoMFA was overlaid on the amino acids in the substrate-binding pocket of the homology model of AST IV and found to show a good fit. Additionally external validation was obtained by using the CoMFA model to design substrates that show high activities. These results establish a methodology for prediction of the substrate specificity of this sulfotransferase based on CoMFA methods that are guided by both the homology model and the catalytic mechanism of the enzyme.

Analytical, structural and metabolic biochemistry

Biological and medical sciences

Enzymes and enzyme inhibitors

Fundamental and applied biological sciences. Psychology

Transferases

Details

Title: Subtitle: Comparative Molecular Field Analysis of substrates for an Aryl sulfotransferase based on catalytic mechanism and protein homology modeling
Creators: Vyas Sharma - University of Iowa
Michael W Duffel - University of Iowa
Resource Type: Journal article
Publication Details: Journal of medicinal chemistry, Vol.45(25), pp.5514-5522
Publisher: American Chemical Society
DOI: 10.1021/jm010481c
PMID: 12459019
ISSN: 0022-2623
eISSN: 1520-4804
Language: English
Date published: 2002
Academic Unit: Pharmaceutical Sciences and Experimental Therapeutics; Medicinal and Natural Products Chemistry
Record Identifier: 9984303286002771

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