Your search keyword '"Guarnera, Enrico"' showing total 5 results

1. AlloMAPS: allosteric mutation analysis and polymorphism of signaling database

Author

Wah Tan, Zhen, Tee, Wei-Ven, Guarnera, Enrico, Booth, Lauren, Berezovsky, Igor N, Wah Tan, Zhen, Tee, Wei-Ven, Guarnera, Enrico, Booth, Lauren, and Berezovsky, Igor N

Abstract

AlloMAPS database provides data on the causality and energetics of allosteric communication obtained with the structure-based statistical mechanical model of allostery (SBSMMA). The database contains data on allosteric signaling in three sets of proteins and protein chains: (i) 46 proteins with comprehensively annotated functional and allosteric sites; (ii) 1908 protein chains from PDBselect set of chains with low (<25%) sequence identity; (iii) 33 proteins with more than 50 known pathological SNPs in each molecule. In addition to energetics of allosteric signaling between known functional and regulatory sites, allosteric modulation caused by the binding to these sites, by SNPs, and by mutations designated by the user can be explored. Allosteric Signaling Maps (ASMs), which are produced via the exhaustive computational scanning for stabilizing and destabilizing mutations and for the modulation range caused by the sequence position are available for each protein/protein chain in the database. We propose to use this database for evaluating the effects of allosteric signaling in the search for latent regulatory sites and in the design of allosteric sites and effectors. The database is freely available at: http://allomaps.bii.a-star.edu.sg.

Published

2019

2. AlloMAPS 2: allosteric fingerprints of the AlphaFold and Pfam-trRosetta predicted structures for engineering and design.

Author

Tan ZW, Tee WV, Guarnera E, and Berezovsky IN

Subjects

Allosteric Regulation genetics, Mutation, Drug Design, Databases, Protein, Proteins chemistry, Signal Transduction

Abstract

AlloMAPS 2 is an update of the Allosteric Mutation Analysis and Polymorphism of Signalling database, which contains data on allosteric communication obtained for predicted structures in the AlphaFold database (AFDB) and trRosetta-predicted Pfam domains. The data update contains Allosteric Signalling Maps (ASMs) and Allosteric Probing Maps (APMs) quantifying allosteric effects of mutations and of small probe binding, respectively. To ensure quality of the ASMs and APMs, we performed careful and accurate selection of protein sets containing high-quality predicted structures in both databases for each organism/structure, and the data is available for browsing and download. The data for remaining structures are available for download and should be used at user's discretion and responsibility. We believe these massive data can facilitate both diagnostics and drug design within the precision medicine paradigm. Specifically, it can be instrumental in the analysis of allosteric effects of pathological and rescue mutations, providing starting points for fragment-based design of allosteric effectors. The exhaustive character of allosteric signalling and probing fingerprints will be also useful in future developments of corresponding machine learning applications. The database is freely available at: http://allomaps.bii.a-star.edu.sg., (© The Author(s) 2022. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2023

3. AlloSigMA 2: paving the way to designing allosteric effectors and to exploring allosteric effects of mutations.

Author

Tan ZW, Guarnera E, Tee WV, and Berezovsky IN

Subjects

Allosteric Regulation, Allosteric Site, Ligands, Models, Molecular, Models, Statistical, Proteins metabolism, Mutation, Proteins chemistry, Proteins genetics, Software

Abstract

The AlloSigMA 2 server provides an interactive platform for exploring the allosteric signaling caused by ligand binding and/or mutations, for analyzing the allosteric effects of mutations and for detecting potential cancer drivers and pathogenic nsSNPs. It can also be used for searching latent allosteric sites and for computationally designing allosteric effectors for these sites with required agonist/antagonist activity. The server is based on the implementation of the Structure-Based Statistical Mechanical Model of Allostery (SBSMMA), which allows one to evaluate the allosteric free energy as a result of the perturbation at per-residue resolution. The Allosteric Signaling Map (ASM) providing a comprehensive residue-by-residue allosteric control over the protein activity can be obtained for any structure of interest. The Allosteric Probing Map (APM), in turn, allows one to perform the fragment-based-like computational design experiment aimed at finding leads for potential allosteric effectors. The server can be instrumental in elucidating of allosteric mechanisms and actions of allosteric mutations, and in the efforts on design of new elements of allosteric control. The server is freely available at: http://allosigma.bii.a-star.edu.sg., (© The Author(s) 2020. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2020

4. AlloMAPS: allosteric mutation analysis and polymorphism of signaling database.

Author

Tan ZW, Tee WV, Guarnera E, Booth L, and Berezovsky IN

Subjects

Allosteric Site genetics, Animals, Genetic Diseases, Inborn genetics, Humans, Internet, Models, Chemical, Models, Molecular, Protein Conformation, Structure-Activity Relationship, Allosteric Regulation genetics, Databases, Protein, Mutation, Polymorphism, Single Nucleotide, Signal Transduction genetics

Abstract

AlloMAPS database provides data on the causality and energetics of allosteric communication obtained with the structure-based statistical mechanical model of allostery (SBSMMA). The database contains data on allosteric signaling in three sets of proteins and protein chains: (i) 46 proteins with comprehensively annotated functional and allosteric sites; (ii) 1908 protein chains from PDBselect set of chains with low (<25%) sequence identity; (iii) 33 proteins with more than 50 known pathological SNPs in each molecule. In addition to energetics of allosteric signaling between known functional and regulatory sites, allosteric modulation caused by the binding to these sites, by SNPs, and by mutations designated by the user can be explored. Allosteric Signaling Maps (ASMs), which are produced via the exhaustive computational scanning for stabilizing and destabilizing mutations and for the modulation range caused by the sequence position are available for each protein/protein chain in the database. We propose to use this database for evaluating the effects of allosteric signaling in the search for latent regulatory sites and in the design of allosteric sites and effectors. The database is freely available at: http://allomaps.bii.a-star.edu.sg.

Published

2019

5. AlloSigMA: allosteric signaling and mutation analysis server.

Author

Guarnera E, Tan ZW, Zheng Z, and Berezovsky IN

Subjects

Allosteric Regulation, Ligands, Models, Molecular, Models, Statistical, Protein Binding, Proteins metabolism, Allosteric Site, Computational Biology methods, Mutation, Signal Transduction

Abstract

Motivation: Allostery is an omnipresent mechanism of the function modulation in proteins via either effector binding or mutations in the exosites. Despite the growing number of online servers and databases devoted to prediction/classification of allosteric sites and their characteristics, there is a lack of resources for an efficient and quick estimation of the causality and energetics of allosteric communication., Results: The AlloSigMA server implements a unique approach on the basis of the recently introduced structure-based statistical mechanical models of allosteric signaling. It provides an interactive framework for estimating the allosteric free energy as a result of the ligand(s) binding, mutation(s) and their combinations. Latent regulatory exosites and allosteric effect of mutations can be detected and explored, facilitating the research efforts in protein engineering and allosteric drug design., Availability and Implementation: The AlloSigMA server is freely available at http://allosigma.bii.a-star.edu.sg/home/., Contact: igorb@bii.a-star.edu.sg., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com)

Published

2017