Books

Docking Screens for Drug Discovery

SpringerDocking Screens for Drug Discovery. Editor: de Azevedo Jr., Walter Filgueira (Ed.)

 

Progress in Cell Cycle Research

 

Springer

Progress in Cell Cycle Research: Volume 2

 

 

Projects

SAnDReS

SAnDReS-SigmaSAnDReS: Statistical Analysis of Docking Results and Scoring functions

 

SFSXplorer

 

SFSXplorer

SFSXplorer: Scoring Function Space eXplorer

 

Taba

TabaTaba: A Tool to Analyze the Binding Affinity

 

Citation

Citation Metrics

Citation Metrics

Citation Metrics

 

Editorships

Current Drug Targets

Frontiers Section Editor (Bioinformatics and Biophysics) for the Current Drug Targets ISSN: 1873-5592

Bentham Link

Current Medicinal Chemistry

Section Editor (Bioinformatics in Drug Design and Discovery) for the Current Medicinal Chemistry ISSN: 1875-533X

Bentham Link

Journal of Molecular Structure

Member of the Editorial Board of the Journal of Molecular Structure ISSN: 0022-2860

Journal of Molecular Structure Link

Molecular Diversity

Member of the Editorial Board of Molecular Diversity ISSN: 1381-1991 (Print) 1573-501X (Online)

Molecular Diversity Link

Exploration of Drug Science

Associate Editor for Exploration of Drug Science

Exploration of Drug Science Link

Frontiers in Chemistry

Reviewer Editor for Frontiers in Chemistry ISSN: 2296-2646

Frontiers in Chemistry Link

Organic and Medicinal Chemistry International Journal

Member of the Editorial Board for the Organic and Medicinal Chemistry International Journal ISSN: 2474-7610

Bentham Link

Bioengineering International

Section Editor in Chief (Bioinformatics) for Bioengineering International. ISSN 2668-7119

Bioengineering International

 

Dr. Walter F. de Azevedo, Jr. has been ranked among the most influential researchers in the world according to a database created by Journal Plos Biology (see news here). Dr. Azevedo`s influential works can be found here. Citation metrics available here.    

Exploring the Scoring Function Space [>>]

We envisage protein-ligand interaction as a result of the relation between the protein space (Smith, 1970Hou et al., 2005) and the chemical space (Bohacek et al., 1996; Dobson, 2004Kirkpatrick & Ellis, 2004; Lipinski & Hopkins, 2004Shoichet, 2004; Stockwell, 2004), and we propose to approach these sets as a unique complex system, where the application of computational methodologies could contribute to understand the structural basis for the specificity of ligands for proteins. Such approaches have the potential to create novel scoring functions to predict binding affinity with superior predictive power when compared with standard methodologies. We propose to use the abstraction of a mathematical space composed of infinite computational models to predict ligand-binding affinity, named here as scoring function space (Heck et al., 2017; Bitencourt-Ferreira & de Azevedo Jr., 2019). By the use of supervised machine learning techniques, we can explore this scoring function space to build a computational model targeted to a specific biological system. For instance, we created targeted-scoring functions for HIV-1 Protease and Cyclin-Dependent Kinases. We developed the programs SAnDReS (Xavier et al., 2016), SFSXplorer, and Taba (da Silva et al., 2020to generate computational models to predict ligand-binding affinity. These programs are integrated computational tools to explore the scoring function space. 

          A view of the scoring function space as a way to develop a computational model to predict ligand-binding affinity.  

Contact

If you have interest in participating in our research projects, please feel free to contact Dr. Walter F. de Azevedo, Jr.

e-mail: walter@azevedolab.net