PDBSite: a database of the 3D structure of protein functional sites

Иванисенко, В. А.; Pintus, Sergey S.; Grigorovich, D. A.; Колчанов, Н. А.

doi:10.1093/nar/gki105

Cited by 71 publications

(50 citation statements)

References 30 publications

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“…All the PDB files with the 3D protein structures 14 and their classification into enzymes or nonenzymes were taken from the literature. 4 The aforementioned descriptors were subsequently used to carry out a LDA with a random training subset of proteins to classify each one of them as enzyme or nonenzyme.…”

Section: Resultsmentioning

confidence: 99%

“…All the PDB files with the 3D protein structures 14 and their classification into enzymes or nonenzymes were taken from the literature. 3 Before collecting the PDB files we perform the calculation of the electrostatic potentials, electrostatic entropy, and electrostatic spectral moments as well as vdW potentials, vdW entropy, vdW spectral moments, HINT potentials, HINT entropy, and HINT spectral moments.…”

Section: Datasetmentioning

confidence: 99%

See 1 more Smart Citation

Computational chemistry study of 3D‐structure‐function relationships for enzymes based on Markov models for protein electrostatic, HINT, and van der Waals potentials

et al. 2008

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In a significant work, Dobson and Doig (J Mol Biol 2003, 330, 771) illustrated protein prediction as enzymatic or not from spatial structure without resorting to alignments. They used 52 protein features and a nonlinear support vector machine model to classify more than 1000 proteins collected from the PDB with a 77% overall accuracy. The most useful features were: the secondary-structure content, the amino acid frequencies, the number of disulphide bonds, and the largest cleft size. Working on the same dataset used by D&D, in this article we reported a good and simple model, based on the Markov chain models (MCM), to classify protein 3D structures as enzymatic or not, taking into consideration the spatial structure without resorting to alignments. Here we define, for the first time, a general MCM to calculate the electrostatic potential, molecular vibrations, van der Waals (vdw) interactions, and hydrophobic interactions (HINT) and use them in comparative studies of potential fields and/or protein function prediction. The dataset is composed of 1371 proteins divided into 689 enzymes and 682 nonenzymes, all proteins were collected from the PDB. The best model we found was a linear model carried out with the linear discriminant analysis; it was able to classify 74.18% of the proteins using only two electrostatic potentials. In the work described here, we define 3D-HINT potentials (mu(k)) and use them for the first time to derive a classifier for protein enzymes. We analyzed ROC curves, domain of applicability, parametric assumptions, desirability maps, and also tested other nonlinear artificial neural network models which did not improve the linear model. In closing, this MCM allows a fast calculation and comparison of different potentials deriving into accurate protein 3D structure-function relationships, notably simpler than the previous.

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Section: Resultsmentioning

confidence: 99%

Section: Datasetmentioning

confidence: 99%

Computational chemistry study of 3D‐structure‐function relationships for enzymes based on Markov models for protein electrostatic, HINT, and van der Waals potentials

et al. 2008

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“…The data points in black squares are from complexes with K d data, and gray diamonds are used for complexes with K i or IC 50 data. [11,15,25,32,33,[41][42][43][44][45][46][47][48][49][50][51][52][53][54][55], but now, we will be able to add another layer of depth to such studies. There is more to binding affinity than just burying a ligand inside a protein, and all of the complex issues that go into creating an effective scoring function [56] will need to be considered in our analyses.…”

Section: Discussionmentioning

confidence: 99%

“…Patterns of valid versus invalid ligands of both types should help current efforts in the field to identify binding sites in apo structures. At this time, groups are focusing on the analysis of occupied versus unoccupied pockets and having good success [11,32,33,[41][42][43][44][45][46][47][48][49], but the methods could be further refined with data on the invalid ligands identified within Binding MOAD.…”

Section: Mining Binding Moadmentioning

confidence: 99%

Exploring protein–ligand recognition with Binding MOAD

Smith

Falkner

et al. 2006

Journal of Molecular Graphics and Modelling

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“…The presence of transmembrane helices was predicted by SOSUI (Hirokawa et al, 1998) and TMHMM (Krogh et al, 2001). Protein 3D-structures were assigned by the Genome to Protein structure and function (GTOP) pipeline (Kawabata et al, 2002), where reverse PSI-BLAST, a variant of the PSI-BLAST algorithm (Altschul et al, 1997) is used for searching of the amino acid sequences derived from the H-Inv cDNA against the PDB database (Ivanisenko et al, 2005).…”

Section: H-invdb Annotation and Advanced Annotationmentioning

confidence: 99%