Ángel R. Ortíz scite author profile

Advances in structural genomics and protein structure prediction require the design of automatic, fast, objective, and well benchmarked methods capable of comparing and assessing the similarity of lowresolution three-dimensional structures, via experimental or theoretical approaches. Here, a new method for sequence-independent structural alignment is presented that allows comparison of an experimental protein structure with an arbitrary low-resolution protein tertiary model. The heuristic algorithm is given and then used to show that it can describe random structural alignments of proteins with different folds with good accuracy by an extreme value distribution. From this observation, a structural similarity score between two proteins or two different conformations of the same protein is derived from the likelihood of obtaining a given structural alignment by chance. The performance of the derived score is then compared with well established, consensus manual-based scores and data sets. We found that the new approach correlates better than other tools with the gold standard provided by a human evaluator. Timings indicate that the algorithm is fast enough for routine use with large databases of protein models. Overall, our results indicate that the new program (MAMMOTH) will be a good tool for protein structure comparisons in structural genomics applications. MAMMOTH is available from our web site at

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MONSSTER: a method for folding globular proteins with a small number of distance restraints

Skolnick

Koliński

Ortíz

1997

Journal of Molecular Biology

251

238

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Prediction of Drug Binding Affinities by Comparative Binding Energy Analysis

Ortíz¹,

Pisabarro²,

Gago³

et al. 1995

J. Med. Chem.

252

241

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A new computational method for deducing quantitative structure-activity relationships (QSARs) using structural data from ligand-macromolecule complexes is presented. First, the ligand-macromolecule interaction energy is computed for a set of ligands using molecular mechanics calculations. Then, by selecting and scaling components of the ligand-macromolecule interaction energy that show good predictive ability, a regression equation is obtained in which activity is correlated with the interaction energies of parts of the ligands and key regions of the macromolecule. Application to the interaction of the human synovial fluid phospholipase A2 with 26 inhibitors indicates that the derived QSAR has good predictive ability and provides insight into the mechanism of enzyme inhibition. The method, which we term comparative binding energy (COMBINE) analysis, is expected to be applicable to ligand-receptor interactions in a range of contexts including rational drug design, host-guest systems, and protein engineering.

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A new progressive-iterative algorithm for multiple structure alignment

Lupyan¹,

Leo‐Macias²,

Ortíz³

2005

131

141

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Ángel R. Ortíz

MAMMOTH (Matching molecular models obtained from theory): An automated method for model comparison

MONSSTER: a method for folding globular proteins with a small number of distance restraints

Prediction of Drug Binding Affinities by Comparative Binding Energy Analysis

A new progressive-iterative algorithm for multiple structure alignment

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